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Clinical guidelines for the Queensland workers’ compensation scheme Psychiatric conditions Contents Before you start Relevance to the workers’ compensation sector............................................................................................................................. 2 Agree appraisal .......................................................................................................................................................................................... 3 Register of clinical practice guidelines for psychiatric conditions ............................................................................................... 4 Click to the relevant guideline Anxiety disorders...................................................................................................................................................................................... 5 Stress related conditions and other mental disorders ................................................................................................................. 15 Practice guideline for the treatment of acute stress disorder sand post traumatic stress disorder .............................. 25 Post-traumatic stress disorder. The management of PTSD in adults and children in primary and secondary care ... 35 Anxiety: Management of anxiety (panic disorder, with or without out agoraphobia, and generalised anxiety disorder) in adults in primary, secondary and community care ................................................................................................ 47 Guideline for the evaluation and treatment of injured workers with psychiatric conditions ............................................ 66 VA/DoD clinical practice guideline for the management of post-traumatic stress ............................................................ 72 © State Government of Queensland (Q-COMP) 2008 The information provided in this publication is distributed by Q-COMP as an information source only. The information is provided solely on the basis that readers will be responsible for making their own assessment of the matters discussed herein and are advised to verify all relevant representations, statements and information. At Q-COMP, our privacy policy applies the Queensland Government’s Information Privacy Principles for the collection, storage, use and disclosure of personal information. Q-COMP uses your personal information for the purposes for which it was collected and will not disclose it to a third party without your consent unless required or authorised to do so by law. If you have any questions about your privacy please contact Q-COMP’s Privacy Officer on 1300 361 235. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Foreword Clinical guidelines for the Queensland workers’ compensation scheme is a selection of clinical guidelines or ‘treatment protocols’ used by other jurisdictions and medical bodies. Q-COMP compiled this selection to create a resource for clinicians treating injured workers in Queensland. Over the course of our research it became clear what type of guidelines are successfully applied to practice and what we should include. They include guidelines where: • • • • • • • medical providers were consulted nurse and allied health providers identified relevant areas to include medical specialty groups endorsed the guidelines an effective promotion program was used patient education brochures or fact sheets for General Practitioners to provide to their patients were developed an education strategy included the Continuing Professional Development (CPD) program frameworks for evaluating the guidelines effectiveness were developed ahead or simultaneously with the guidelines themselves. I am looking forward to receiving your feedback on Clinical guidelines for the Queensland workers’ compensation scheme and your support in achieving the best outcomes for injured workers in Queensland. Elizabeth Woods Chief Executive Officer Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 1 2 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 16 5 4 1 1 1 8 3 1 3 1 7 2 1 1 3 5 Anxiety Management of anxiety (panic disorder, with or without agoraphobia, and generalised anxiety disorder) in adults in primary, secondary and community care 5 1 2 1 1 Guideline for the evaluation and treatment of injured workers with psychiatric conditions. 6 10 2 1 3 4 VA/DoD clinical practice guideline for the management of post-traumatic stress 7 Rating criteria CPG 1 and CPG 3 have the highest rating score. This is due to their higher scores in all four of the categories. Both CPG 5 and CPG 6 rate less than CPG1 and CPG 3 on the Psychological factors, but are high in at least two of the other categories. 5 1 To what degree does the guideline consider Risk Factors for Recovery? Total Score 4 4 1 1 1 Anxiety disorders 3 Stress related conditions and other mental disorders 2 Post-traumatic stress disorder. The management of PTSD in adults and children in primary and secondary care Practice guideline for the treatment of acute stress disorders and post traumatic stress disorder. To what degree does the guideline consider the Return to Work Process (vocational rehabilitation)? Risk Factors for Recovery To what degree does the guideline consider psychosocial factors that may influence recovery? Return to Work Process (vocational rehabilitation) Does the guideline consider graded increases in activity and function? Psychosocial Factors Functional Restoration 4 3 2 1 Each item is rated on a 5-point scale ranging from 5 “Strongly Agree” to 1 “Strongly Disagree”. The scale measures the extent to which a criterion (item) has been fulfilled. Relevance to the workers compensation sector Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 3 Scope and Purpose Stakeholder Involvement Rigour of Development Clarity and Presentation Applicability Editorial Independence 56% 29% 47% 63% 11% 17% 46% 36% 46% 0% 17% Stress related conditions and other mental disorders 2 72% Anxiety disorders 1 4 67% 0% 50% 57% 42% 67% 8% 67% 2% 0% 79% 2% Post-traumatic Practice guideline stress disorder. for the treatment The management of acute stress of PTSD in adults disorders and post and children traumatic stress in primary and disorder. secondary care 3 42% 44% 83% 48% 79% 72% 5 Anxiety Management of anxiety (panic disorder, with or without agoraphobia, and generalised anxiety disorder) in adults in primary, secondary and community care 25% 0% 36% 24% 36% 61% Guideline for the evaluation and treatment of injured workers with psychiatric conditions. 6 17% 11% 92% 60% 46% 67% VA/DoD clinical practice guideline for the management of post-traumatic stress 7 Each item is rated on a 5-point scale ranging from 5 “Strongly Agree” to 1 “Strongly Disagree”. The scale measures the extent to which a criterion (item) has been fulfilled. The aggregate scores are then converted into a percentage scale ranging from 100%” Strongly Agree” to 1% “Strongly Disagree”. Agree appraisal Register of clinical practice guidelines for psychiatric conditions CPG 1 Name Anxiety disorders Source National Guideline Clearinghouse www.guideline.gov 2 3 4 5 6 7 4 Stress related conditions and other mental disorders National Guideline Clearinghouse Practice guideline for the treatment of acute stress disorders and post traumatic stress disorder. Post-traumatic stress disorder. The management of PTSD in adults and children in primary and secondary care Anxiety - Management of anxiety (panic disorder, with or without agoraphobia, and generalised anxiety disorder) in adults in primary, secondary and community care Guideline for the evaluation and treatment of injured workers with psychiatric conditions. National Guideline Clearinghouse VA/DoD clinical practice guideline for the management of post-traumatic stress www.guideline.gov Developed by Singapore Ministry of Health, National Medical Research Council. Anxiety disorders. Singapore: Singapore Ministry of Health;2003 Nov.69 p. [74 references] Work Loss Data Institute. Stress related conditions and other mental disorders. Corpus Christi (TX): Work Loss Data Institute; 2006.91 p. [128 references] American Psychiatric Association. Practice guideline for the treatment of patients with acute stress disorder and post traumatic stress disorder. Arlington (VA); American www.guideline.gov Psychiatric Association :2004 Nov.57 p. [463 references] National Guideline Clearinghouse National Collaborating Centre for Mental Health. Posttraumatic stress disorder: the management of PTSD in adults and children in primary and secondary care. www.guideline.gov London (UK): National Institute for Clinical Excellence (NICE);2005.167 p. [69 references] National Guideline Clearinghouse National Collaborating Centre for Primary Care - National Institute for Clinical Excellence London 2004 www.guideline.gov National Guideline Clearinghouse Washington State Department of Labor and Industries. Guideline for the evaluation and treatment of injured workers with psychiatric conditions. Olympia (WA) : www.guideline.gov Washington State Department of Labor and Industries; National Guideline 2004 .6 p. Clearinghouse www.guideline.gov National Guideline Veterans Health Administration, Department of Defence. Clearinghouse VA/DoD clinical practice guideline for the management of post-traumatic stress. Version 1.0. Washington www.guideline.gov (DC): Veterans Health Administration , Department of Defense;2004 Jan. Various p. [479 references] Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Anxiety disorders Contents 1. 2. 3. 4. 5. 6. 7. Developed by ...................................................................................................................................................................................... 6 Guideline status .................................................................................................................................................................................. 6 Where located/how accessed ........................................................................................................................................................ 6 Description/scope ............................................................................................................................................................................. 6 Outcomes considered ....................................................................................................................................................................... 8 Agree appraisal.................................................................................................................................................................................... 8 Relevance/appropriateness of use in workers’ compensation sector .................................................................................. 8 a) Functional progression ............................................................................................................................................................... 8 b) Physical/psychiatric rehabilitation ........................................................................................................................................ 12 c) Risk factor/recovery ................................................................................................................................................................ 13 d) Return to work........................................................................................................................................................................... 14 8. Priority for Q-COMP ...................................................................................................................................................................... 14 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 5 1. Developed by Singapore Ministry of Health, National Medical Research Council. Anxiety disorders. Singapore: Singapore Ministry of Health; 2003 Nov.69 p. [74 references] 2. Guideline status This is the current release of the guideline. 3. Where located/how accessed National Guideline Clearinghouse www.guideline.gov Electronic copies; Available in Portable Document Format (PDF) from the Singapore Ministry of Health Web Site Print copies; Available from the Singapore Ministry of Health, College of Medicine Building, Mezzanine Floor 16 College Rd, Singapore 169854 4. Description/scope Disease/condition(s) • Anxiety disorders • Panic disorder • Agoraphobia • Specific phobias • Social anxiety disorder (SAD, social phobias) • Generalized anxiety disorder • Obsessive-compulsive disorder • Post-traumatic stress disorder Guideline category • Counselling • Diagnosis • Evaluation • Management • Treatment Clinical speciality • Family Practice • Psychiatry • Psychology Intended users • Allied Health Personnel • Physicians • Psychologists/ Non-physician Behavioural Health Clinicians • Social Workers 6 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Guideline objectives 1. To provide optimal care and good outcomes to patients with anxiety disorders 2. To assist primary health care physicians in clinical decision-making when assessing and treating patients with anxiety 3. To help medical practitioners recognise the presence of anxiety disorders in patients and to assess and manage them appropriately 4. To provide evidence-based recommendations on appropriate psychological and pharmacological therapy for anxiety. Target population Adults and children with anxiety disorders in Singapore Interventions and practices considered Diagnosis and assessment 1. Evaluation of symptoms: psychotic symptoms , severity/ complexity of symptoms, and severity of functional impairment 2. Evaluation and mobilization of family and social resources 3. Assessment for suicide risk 4. Assessment for coexisting mental health disorders such as depression and drug/alcohol problems 5. Patient response to treatment: monitoring for remission and relapse. Treatment: Non-pharmacotherapy 1. Supportive counselling and monitoring: reassuring patient; educating patient, including providing information on treatment options 2. Lifestyle changes: stress reduction strategies; reducing alcohol and caffeine ; avoiding nicotine and drug use; regular exercise 3. Group therapy 4. Referral to psychiatrist or other behavioural treatment specialist 5. Psychotherapy • Cognitive behaviour therapy (CBT), including psychoeducation; exposure to symptoms or situations; cognitive restructuring; breathing retraining; continuous panic monitoring. • Other psychotherapies Treatment: Pharmacotherapy 1. Antidepressants • Selective serotonin reuptake inhibitors (SSRIs )as first-line drug treatment, including citalopram, fluoxetine, fluvoxamine, sertraline, and paroxetine • Tricyclic antidepressants including imipramine and clomipramine • Monoamine oxidase inhibitor (MAOIs) such as phenelazine and tranylcypromine • Selective reversible inhibitor of MAO type A (RIMA) (moclobemide) 2. Benzodiazepines: alprazolam, bromazepam, clonazepam, diazepam, lorazepam 3. Beta-blockers, such as propanolol and atenolol 4. Venlafaxine, a serotonin norepinephrine reuptake inhibitor (SNRI) 5. Serotonin antagonist and reuptake inhibitor (nefazadone) and noradrenergic and serotonin antagonist (mirtazapine) 6. Antihistamine (hydroxyzine) Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 7 5. Outcomes considered • • • • • Symptoms of anxiety disorders Morbidity and overall functioning Effectiveness of counselling and behavioural therapies Effectiveness of safety of medications Side effects, adverse reactions, and potential interactions of medications 6. Agree appraisal • • • • • • Scope and Purpose Stakeholder Involvement Rigour of Development Clarity and Presentation Applicability Editorial Independence 72% 46% 36% 46% 0% 17% 7. Relevance/appropriateness of use in workers’ compensation sector a) Functional progression No specific functional progression stated Two clinical algorithms are provided in the original guideline document for: • Diagnosing Anxiety Disorders • Treatment of Anxiety Disorders Major recommendations The recommendations that follow are those from the guideline´s executive summary; detailed recommendations can be found in the original guideline document. Treatment settings for anxiety disorders Helpful immediate steps that can be instituted at the primary care level include (“Practice guideline for the treatment of patients with panic disorder,” 1998): • Evaluating particular symptoms and performing a diagnostic evaluation, in order to arrive at a provisional diagnosis of an anxiety disorder • Evaluating the type and severity of functional impairment • Establishing and maintaining a therapeutic alliance with the patient based upon empathy and understanding • Educating the patient about the nature and origin of their anxiety symptoms and appropriate reassurance (e.g., that they are not having a “heart attack” or are “going crazy”) • Evaluation and mobilization of family and social resources to aid the patient • Suggestion of lifestyle changes as appropriate • Stress reduction strategies • Reducing alcohol and caffeine • Avoiding nicotine and drug use • Regular exercise • Supportive counseling 8 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions • Symptomatic relief with medication prescribed on a short-term basis • Monitoring over time and addressing early signs of relapse. Psychiatric evaluation and treatment is appropriate when • • • • • There is serious risk of suicide There are psychotic symptoms Cooccurring drug/alcohol problems exist Symptoms are severe/complex If symptoms fail to improve on initial treatment and follow-up Psychosocial interventions for anxiety disorders Psychological therapy should be routinely considered as a treatment option when assessing mental health problems, including anxiety disorder. Patients should be informed about all available forms of treatment, including psychological therapies, and their preference for the type of treatment should be taken into account when considering the overall treatment plan (“Practice guideline for the treatment of patients with panic disorder,” 1998). Medications for anxiety disorders Pharmacological treatment is indicated when: • Symptoms are severe • There is significant impairment of social, occupational and role functioning • There is concurrent moderate or severe depressive disorder (“Practice guideline for the treatment of patients with panic disorder,” 1998). Antidepressants Antidepressants are recommended as effective agents for the treatment of panic disorders, social phobia, obsessive compulsive disorders, generalized anxiety disorder, and post-traumatic stress disorder. Selective serotonin reuptake inhibitors (SSRIs) are recommended as first-line drug treatment for anxiety disorder. Benzodiazepines The lowest effective dose to achieve symptom relief should be used over a limited period. The dose should be gradually tapered off. Long-term use should be closely supervised for adverse effects, abuse, tolerance, dependency, and withdrawal symptoms (“Guidelines for prescribing benzodiazepines,” 2002; “College Guidelines for use of benzodiazepines,” 1999; “Benzodiazepines: risks, benefits or dependence,” 1997). Treatments for different types of anxiety disorders Panic Disorder For panic disorder, high potency agents like alprazolam and clonazepam are effective in providing rapid relief. With discontinuation of these agents, however, patients should be closely monitored for recurrence of symptoms, as the rates of relapse are very high, especially for shorter-acting agents (Noyes et al., 1991). Almost all the SSRIs (fluoxetine, sertraline, fluvoxamine, citalopram, paroxetine) have documented efficacy in the treatment of panic disorder (Otto et al, 2001). Imipramine is effective in the treatment of panic disorder. An optimal effective dose for treatment is 100 to 225 mg and should be continued for 8 to 12 weeks (“Drug treatment of panic disorder,” 1992; Mavissakalian & Perel, 1989). Clomipramine is effective for panic disorder at a dose of 50 to 100 mg for a duration of 6 to 12 weeks (Cassano et al., 1988). Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 9 Cognitive behaviour therapy (CBT) is the psychotherapy of choice for panic disorder. Possible treatment components for panic disorder, with or without agoraphobia, are (“Practice guideline for the treatment of patients with panic disorder,” 1998; Clum, Clum, & Surls, 1993; Clark et al, 1994; Trull, Nietze, & Main, 1988): • • • • • Psychoeducation Exposure to symptoms or situations Cognitive restructuring Breathing retraining Continuous panic monitoring Specific Phobias Phobic symptoms respond best to exposure therapy to the feared situation or object (Dupont, 1982; Park et al., 2001). Beta-blockers are effective for specific and circumscribed performance anxiety, especially for patients with prominent sympathetic hyperarousal such as palpitations and tremor. Propranolol 10 to 40 mg taken 45 to 60 minutes before the performance is sufficient for most patients (Tyrer, 1988). Social Anxiety Disorder (Social Phobia) Cognitive behaviour therapy (CBT) is recommended as effective treatment for social anxiety disorder. Exposure to feared situations is a crucial component. Group approaches are useful and often include elements of social skills training. SSRI antidepressants are effective for the treatment of social phobia, and their favourable side-effect profile make them recommended first-line treatment for social phobia. Paroxetine has been the most extensively studied SSRI for social phobia (Leibowitz et al., “A randomized, double-blind, fixed dose comparison of paroxetine,” 2002). There is limited support for the use of moclobemide for social anxiety disorder (SAD) (Stein et al., 2002). Generalised Anxiety Disorder Cognitive behaviour therapy in generalised anxiety disorder delivered by experienced therapists shows good evidence of efficacy. Two-thirds of patients show clinically significant improvement at 6 months follow-up (Durham et al, 2003; Borkovec & Costello, 1993). Imipramine for 3 to 6 months is recommended for treating generalized anxiety disorder (GAD) (Rickels et al, 2000). Paroxetine has shown efficacy compared to placebo for GAD treatment (Stocchi et al., 2003). Venlafaxine, a serotonin norepinephrine reuptake inhibitor (SNRI) has been shown to be effective in GAD (Gelenberg et al., 2000). Serotonin antagonist and reuptake inhibitors such as nefazodone and the noradrenergic and serotonin selective antagonist mirtazapine may have useful anxiolytic effects in GAD (Goodnick et al., 1999; Hedges et al., 1996). Antidepressants can be considered as first-line agents over benzodiazepines in the treatment of GAD over the long term (Kapczinski et al., 2003). Hydroxyzine 50 mg/day has shown efficacy for treatment of GAD. Obsessive Compulsive Disorder The recommended first line of pharmacotherapy for obsessive compulsive disorder (OCD) is a 10 to 12 week trial with an SSRI at adequate doses. Fluvoxamine, fluoxetine, citalopram, sertraline, and paroxetine, have all been shown to be effective in adults with OCD (Greist et al., 1995). The efficacy of fluvoxamine, fluoxetine, and sertraline in OCD has also been confirmed in children (Cook et al., 2001; Liebowitz et al., “Fluoxetine in children and adolescents,” 2002). 10 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Clomipramine is effective treatment for OCD in the dose range of between 100 to 300 mg/day for a period of 5 to 12 weeks (McDonough & Kennedy, 2002; Mundo, Maina, & Uslenghi, 2000). It has been suggested that an adequate treatment trial in OCD would be for at least 10 to 12 weeks, with a minimum mean daily dosage of one of the following agents: • • • • • Clomipramine 150 mg Fluvoxamine 150 mg Fluoxetine 40 mg Sertraline 150 mg Paroxetine 40 mg Behaviour therapy using Exposure-Response Prevention (ERP) is the treatment of choice for limiting the dysfunction resulting from obsessions and/or compulsions (Van Balkom et al., 1994; O´Sullivan et al., 1991). Post-Traumatic Stress Disorder (PTSD) SSRIs are generally the most appropriate medication of choice for PTSD, and effective therapy should be continued for 12 months or longer. Paroxetine, sertraline, and fluoxetine all have well documented evidence of efficacy (Ballenger et al., 2000). It is not recommended, however, that treatment of PTSD, including medication treatment, be instituted and continued only at the primary care setting, over a long term (Khouzam & Donnelly, 2001). Studies of cognitive behaviour therapy (CBT) have shown the most effective results in the treatment of PTSD. The most appropriate psychotherapy is exposure therapy, and it should be continued for 6 months, with follow-up therapy as needed. Support groups may be beneficial (Ballenger et al., 2000; Davidson & Parker, 2001). Choosing and combining medication and psychosocial interventions Choosing between medications or psychosocial interventions with or without medications should take into account comparable efficacies, differences in risks/benefits, differences in costs, the availability/accessibility of trained therapists and patient preferences (“Practice guideline for the treatment of patients with panic disorder,” 1998). There is evidence that, in the short-term, combined cognitive behaviour therapy with medication does confer additional benefits of faster onset of symptom relief and lasting remission for panic disorder (Lader & Bond, 1998). For panic disorder, recent evidence supports the use of combined cognitive behaviour therapy with medication as superior to either therapy alone in the longer term maintenance phase (Barlow et al., 2000). Anxiety and coexisting conditions Depression, when coexisting with anxiety, should be treated aggressively (Rapaport, 2001; Essau, Conradt, & Petermann, 2002). Antidepressants have good antianxiety properties and should be the medication of choice in comorbid depression and anxiety. Some SSRIs and venlafaxine have demonstrated efficacy for treatment of comorbid depression and anxiety (Ballenger, 1999; Silverstone & Salinas, 2001). Alcohol/substance abuse should be concurrently treated with the anxiety disorder (Tomasson & Vaglum, 1996; LaBounty et al., 1992; Tollefson, Montague- Clouse, & Tollefson, 1992). Benzodiazepines prescribed for anxiety may be abused by some patients with comorbid alcohol/substance abuse/ dependence and are best avoided where possible (Posternak & Mueller, 2001). Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 11 Long-term treatment Long-term maintenance treatment of anxiety disorder is recommended following the amelioration of acute symptoms, as it strongly predicts continued remission following discontinuation of medications (Rickels & Schweizer, 1998). Relapse is common after discontinuation of medication for most anxiety disorders. Maintenance therapy may be indicated for individuals who frequently relapse (Mavissakalian & Perel, 2001). Medication should be continued in OCD treatment for most patients for at least 1 year. The relapse rate with abrupt discontinuation of medication is high, as much as 90% in some studies. A gradual taper of medication over a longer period (e.g. 6 months) is recommended (Ravizza et al., 1996). After improvement with medication, antidepressant treatment for panic disorders and social phobias should be continued for at least 6 months (Michelson et al., 1999; Walker et al., 2000). Similarly for psychological treatments, there is evidence that continuation of therapy sessions during long term follow-up can further lead to improvement and reduce relapse (Ost, 1989). Abrupt discontinuation of benzodiazepines should be avoided. Medication should be tapered off gradually over a number of weeks, titrating against symptoms to avoid withdrawal syndrome and symptom rebound (Pecknold et al., 1988). Longer-acting benzodiazepines are less likely to cause withdrawal and may be used during the tapering period to ameliorate symptoms (Noyes et al, 1991). Gradual tapering of dosage of medication is recommended in discontinuing benzodiazepines after long-term treatment of anxiety disorder (Voshaar et al., 2003). Cognitive behaviour therapy may facilitate the tapering of benzodiazepines (Otto et al., 1993). Discontinuation of antidepressants poses less of a problem in terms of withdrawal symptoms, although changes in mood, affect, appetite, and sleep may occur with SSRI discontinuation, more so with a shorter acting SSRI, such as paroxetine (Lejoyeux & Ades, 1997). Clinical algorithm(s) Two clinical algorithms are provided in the original guideline document for: 1. Diagnosing Anxiety Disorders 2. Treatment of Anxiety Disorders b) Physical/psychiatric rehabilitation As above. 12 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions c) Risk factor/recovery Potential harms Potential side effects and adverse reactions of psychotherapeutic. Medications Benzodiazepines • Dependence, tolerance, and withdrawal symptoms can occur, especially in patients with history of drug dependence. • Central nervous system effects (e.g., sedation, drowsiness, muscle weakness, ataxia. Less commonly, slurred speech, vertigo, headache, confusion). In elderly, risk of confusion and falls. Symptoms decrease after continued use. • Paradoxical excitement can occur. Selective serotonin reuptake inhibitors (SSRIs) • Sexual side effect; cost may be higher compared with other medication classes. Special Instructions: Initial feeling of increased anxiety may occur with SSRIs. Therefore initial dose should be lower than normally prescribed for depression and increased slowly. If discontinued after long-term use, taper dose over several weeks. Use with caution in patients with hepatic or renal dysfunction and in patients with seizure disorders. • Citalopram: Dry mouth, nausea, insomnia, sexual dysfunction, sweating, tremor, diarrhea, somnolence, and dyspepsia. • Fluoxetine: Dose related reactions: nervousness and anxiety, insomnia. Other reactions are headache, nausea, diarrhea, anorexia, blurred vision, sexual dysfunction, drowsiness, sleep disturbance, abnormal dreams, and mania. • Fluvoxamine: Headache, somnolence, insomnia, dizziness, nervousness, nausea, diarrhea, muscle weakness, palpitations, yawning, sexual dysfunction, and tremors. • Paroxetine: Dose related reactions: Somnolence, asthenia, dizziness, tremor, and nausea. Other reactions are headache, insomnia, nervousness, anxiety, dry mouth, constipation, diarrhea, sexual dysfunction, oropharyngeal disorders, and myopathy. • Sertraline: Headache, somnolence, drowsiness, fatigue, dizziness, insomnia, tremor, anxiety, paresthesia, agitation, sexual dysfunction, nausea, dry mouth, diarrhea, constipation, and abnormal vision. Serotonin and Norepinephrine Reuptake Inhibitor (SNRI) • Venlafaxine: Dose related reactions: vasodilation and hypertension. Other reactions are headache, somnolence, dizziness, insomnia, nervousness, nausea, anorexia, constipation, diarrhea, sexual dysfunction, anxiety, abnormal dream, yawning, tremor, and blurred vision. • Special Instructions: If discontinued after long-term use, taper dose over several weeks. Use with caution in renal and hepatic impairment. Tricyclic Antidepressants (TCAs) • Clomipramine and imipramine: Side effects are mostly due to antimuscarinic actions and may be decreased if started at low dose and increased gradually. Dry mouth, constipation (may lead to paralytic ileus), blurred vision, increased intraocular pressure, urinary retention, hyperthermia, drowsiness can occur, nervousness, insomnia, headache, peripheral neuropathy, ataxia, tremor, confusion/delirium can occur especially in older patients, nausea/vomiting, gastric irritation, hypotension, tachycardia, sweating, and weight gain. Risk of cardiovascular and anticholinergic side effects are greater for the elderly or patients with general medical problems. TCAs are suboptimal for suicidal patients because an overdose may be fatal. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 13 • Special Instructions: do not stop medication abruptly; taper dose over several weeks. Use with caution in patients with urinary retention, prostatic hyperplasia, chronicconstipation, untreated angle-closure glaucoma, cardiovascular disease, history of epilepsy, diabetes mellitus, and impaired hepatic function. Elderly patients may be sensitive to side effects; lower dose should be used. Antihistamine • Hydroxyzine: Drowsiness, sedation, dizziness, and lassitude which may diminish over time. Headache, psychomotor impairment, muscarinic side effects, (e.g., dry mouth, blurred vision, urinary retention, constipation, gastroesophageal reflux disease), nausea/vomiting, sweating, and myalgia. Beta Blockers • Atenolol and propranolol: Adverse reactions are not usually significant when only taken on an “as needed” basis. Cardiovascular effects (e.g., bradycardia, hypotension. In patient´s with preexisting cardiovascular disorders: heart block, heart failure), bronchospasm, fatigue, depression, dizziness, and sleep disturbances. May interfere with carbohydrate and lipid metabolism and cause a rash. • Special Instructions: use with caution in patients with asthma, chronic obstructive pulmonary disease, and diabetes mellitus. d) Return to work Not discussed 8. Priority for Q-COMP Rating criteria 14 Functional restoration Does the guideline consider graded increases in activity and function? 2 Psychosocial factors To what degree does the guideline consider psychosocial factors that may influence recovery? 1 Return to work process (vocational rehabilitation) To what degree does the guideline consider the Return to Work Process (vocational rehabilitation)? 1 Risk factors for recovery To what degree does the guideline consider Risk Factors for Recovery? 1 Total rating 5 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Stress related conditions and other mental disorder Contents 1. 2. 3. 4. 5. 6. 7. Developed by ................................................................................................................................................................................... 16 Guideline status ............................................................................................................................................................................... 16 Where located/how accessed ..................................................................................................................................................... 16 Description/scope .......................................................................................................................................................................... 16 Outcomes considered .................................................................................................................................................................... 18 Agree appraisal................................................................................................................................................................................. 18 Relevance/appropriateness of use in workers’ compensation sector ............................................................................... 19 a) Functional progression ............................................................................................................................................................ 19 b) Physical/psychiatric rehabilitation ........................................................................................................................................ 20 c) Risk factor/recovery ................................................................................................................................................................ 20 d) Return to work........................................................................................................................................................................... 20 8. Priority for Q-COMP ...................................................................................................................................................................... 24 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 15 1. Developed by Work Loss Data Institute. Stress related conditions and other mental disorders. Corpus Christi (TX): Work Loss Data Institute; 2006.91 p. [128 references] 2. Guideline status This is the current release of the guideline. This guideline updates a previous version: Work Loss Data Institute. Stress related conditions and other mental disorders. Corpus Christi (TX): Work Loss Data Institute; 2005.104 p. 3. Where located/how accessed National Guideline Clearinghouse www.guideline.gov Electronic copies; Available to subscribers from the Work Loss Data Institute web site Print copies; Available from the Work Loss Data Institute ,169 Saxony Road, Suite 210 Encinitas, CA 92024; Phone 800-488-5548, 760-753-9993, Fax: 760-753-9995; www.worklosdata.com. The following companion documents are available: • Background information on the development of the Official Disability Guidelines of the Work Loss Data Institute is available from the Work Loss Data Institute Web site. • Appendix A. ODG Treatment in Workers’ Comp. Methodology description using the AGREE instrument. Available to subscribers from the Work Loss Data Institute Web site The following patient resources are available: • Appendix B. ODG Treatment in Workers’ Comp. Patient information resources. 2006. Electronic copies: Available to subscribers from the Work Loss Data Institute Web site. Print copies: Available from the Work Loss Data Institute, 169 Saxony Road, Suite 210, Encinitas, CA 92024; Phone: 800-488-5548, 760-753-9992, Fax: 760-753-9995; www.worklossdata.com 4. Description/scope Disease/condition(s) • Work-related stress and other mental disorders Guideline category • Counseling • Diagnosis • Evaluation • Management • Treatment 16 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Clinical speciality • Family Practice • Internal Medicine • Psychiatry • Psychology Intended users • Advanced Practice Nurses • Health Care Providers • Health Plans • Nurses • Physician Assistants • Physicians • Psychologists/ Non-physician Behavioural Health Clinicians Guideline objectives To offer evidence-based step-by-step decision protocols for the assessment and treatment of workers’ compensation conditions. Target population Workers with occupational stress and other mental disorders. Interventions and practices considered The following interventions were considered and recommended as indicated in the original guideline document: 3. 4. 5. 6. Acceptance and commitment therapy (ACT) Activity restrictions/Work modifications Acupressure Antidepressants (the choice of first-line therapy between selective serotonin reuptake inhibitors [SSRIs] and tricyclic antidepressants [TCA] is currently under study) 7. Aromatherapy 8. Cognitive therapy 9. Cognitive behavioural stress management 10. Depression screening 11. Disease management programs 12. Distractive methods 13. Duloxetine (Cymbalta ®) 14. Electroconvulsive therapy 15. Exercise 16. Kava extract 17. Light therapy 18. Massage therapy 19. Mind/body interventions 20. Music 21. Patient education Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 17 22. Peer support 23. Psychological evaluation 24. Psychosocial empowerment programs 25. Return to work 26. St john’s wort 27. Stress inoculation training 28. Stress management , behavioural/cognitive interventions 29. Stress management, physical interventions (aerobic exercise) 30. Therapist optimism 31. Vitamin use (multi-vitamin and mineral supplements) 32. Yoga The following interventions/procedures are under study and are not specifically recommended: 1. Acupuncture 2. Brain wave synchronizers for stress reduction 3. Computer-assisted cognitive therapy 4. Expatriate employee adjustment 5. fatigue (as precursor to stress) 6. Folate 7. Hypnosis 8. Innovative promotion program 9. Opioid antagonist (naltrexone) 10. Pharmaceuticals versus behavioural therapy for tension headaches 11. Psychosocial and pharmacological treatment (for deliberate self harm) 12. SAMe (S-adenosylmethionine) 13. Technological stress The following interventions/procedures were considerd, but are not recommended: 1. Psychological debriefing (for preventing post-traumatic stress disorder) 2. Vitamin B6 5. Outcomes considered Effectiveness of treatments in reducing stress and anxiety. 6. Agree appraisal • • • • • • 18 Scope and Purpose Stakeholder Involvement Rigour of Development Clarity and Presentation Applicability Editorial Independence 56% 29% 47% 63% 11% 17% Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 7. Relevance/appropriateness of use in workers’ compensation sector a) Functional progression Major recommendations Initial diagnosis Stress is the most common mental condition treated by occupational or primary care physicians and will be the focus of this guideline. References to additional mental disorders are found in the procedure summary in the original guideline document, although the more severe of those usually require referral to a specialist. Stress is not its own diagnosis but rather a combination of non-specific emotional or physical symptoms varying in intensity and duration, which may or may not be related to a specific incident. The stress might also be associated with a particular disease or syndrome, but that is not always the case. A stressor is defined as anything that exerts a physical, emotional, or mental demand on an individual. Stress often occurs when the individual has anxiety because of a mismatch between perceived demands and resources, whether work-related or personal. The source of stress can be acute (such as an employee relocation) or chronic (such as consistently poor relations with a supervisor). For some people, stress causes or contributes to a deterioration of physical health, resulting in more headaches or more common colds. While the scientific literature is not clear on this topic, stress may also contribute to the worsening of more serious conditions such as heart disease, irritable bowel disease, or ulcers, depending on the individual’s coping methods. On the other hand, the presence of certain physical conditions could be the cause of stress. Initial evaluation Focus on identifying possible red flags or warning signs for potentially serious psychopathology that would require immediate specialty referral. Red flags may include impairment of mental functions, overwhelming symptoms, signs of substance abuse, or debilitating depression. In the absence of red flags, the occupational or primary care physician can handle most common stress-related conditions safely. In talking to the patient, it is important for the physician to get him or her to try and explain or pinpoint incidents or reasons for the stress, rather than to just generalize (i.e., “I hate my job,” “Everything makes me stressed out”). The physician may have to ask more specific questions about work or home life if the patient is initially unwilling or unable to address specific issues. Occupational stress usually stems from one of three common models: 1. Person-environment fit model: Poor job fit, such as a mismatch between the skills of the individual and the demands of the job, or a disparity between the individual’s career-related desires versus actual opportunities presented, is a leading cause of workplace stress. 2. Demand control model: Jobs that place high demands on the worker but give him or her little control or opportunities for decision-making lead to high job strain, a source of stress that is consistently linked as a contributor to physical conditions such as cardiovascular mortality, heart disease, and hypertension. Consideration should be given to the influence of the individual’s occupational and personal history, which may have an effect on how this model applies to his or her situation. 3. Effort-reward model: Shows that stress is often the result of high effort without social reward. Like the demand control model, this model points out that a low ratio of effort to reward leads to sustained autonomic arousal and can cause physical effects such as high blood pressure or myocardial infraction. Exploration of how and if the patient’s stress follows the path of one of the above models will be helpful in determining treatment. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 19 More specific sources of stress include bereavement, illness, familial changes or disorder, or other common and/or traumatic life changes. Time off work may be helpful, although the ultimate goal should be to preserve the patient’s ability to function both occupationally and socially. Time off should not be so excessive that the employee loses his or her sense of function and appreciation at work and at home. Initial therapy 1. Pursuing the patient’s thoughts on how his or her stress relates to the above models may help determine the source of stress and cultivate ideas on how to eliminate or cope with the stress. Patient education and understanding about stress is necessary for effective stress management to take place. Other common treatment pathways include the use of one or more of the following: a. Relaxation techniques (such as meditation) b. Exercise (aerobic exercise has been shown to positively influence mood) c. Behavioral training (such as time management, anger management, assertiveness, or conflict resolution training) d. Stress inoculation therapy e. Cognitive therapy f. Modified work g. Organizational interventions 2. Pharmaceutical therapy (limited, short-term use of anti-anxiety agents to improve function – anything else should be used in conjunction with a specialty referral) Follow-up visits are an important part of treatment and should be conducted by a mid-level practitioner in person or via phone every three or four days, depending on the severity of the case, while a path to recognizable treatment is established and followed. Failure to improve or make significant progress after several months may indicate the need for psychiatric assessment or counseling. b) Physical/psychiatric rehabilitation As above. c) Risk factor/recovery Potential harms • Despite the relative low prevalence of side effects associated with selective serotonin reuptake inhibitors (SSRIs) a significant minority of older people find these drugs intolerable and experience nausea, vomiting, dizziness and drowsiness. • Hypomania as a potential adverse effect of light therapy needs to be considered. d) Return to work Official Disability Guidelines (ODG) Return-To-Work Pathways Senile and presenile organic psychotic conditions (see original guideline document for International Classification of Diseases, Ninth Revision [ICD-9] codes for this and other diagnoses) Not severe, medical treatment: 0 days Severe, specially designed, limited modified work: 7 days Severe, regular work: indefinite Senile dementia with delusional or depressive features Severe, specially designed, limited modified work: 7 days Severe, affecting fellow worker productivity & safety: indefinite Severe, regular work: indefinite 20 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Alcohol withdrawal delirium Without hospitalization: 1-7 days Including rehab, substance abuse professional (SAP) evaluation: 28 days Including rehab, SAP evaluation, job safety issues: 42 days Drug withdrawal syndrome Without hospitalization: 0-5 days With hospitalization, without suicidal ideation: 7 days With hospitalization, with suicidal ideation: 21 days Paranoid and/or hallucinatory states induced by drugs Without hospitalization: 1-3 days With hospitalization, without threat of harm: 7 days With hospitalization, with threat of harm: 21 days Transient organic psychotic conditions 14 days Paranoid type Without hospitalization, no job safety issues: 0-7 days With hospitalization: 42 days or by report Unspecified schizophrenia Without hospitalization, no job safety issues: 0-7 days With hospitalization: 16-42 days Major depressive disorder, single episode Rule out impaired mood/personality disorder: 0 days Outpatient therapy, without symptoms affecting work: 0-7 days Outpatient therapy, with symptoms interfering with work: 21-42 days With hospitalization, non-cognitive/modified work: 21 days With hospitalization, cognitive work: 42 days Major depressive disorder, recurrent episode Outpatient therapy, without symptoms affecting work: 0-7 days Outpatient therapy, with symptoms interfering with work: 14-28 days With hospitalization, non-cognitive/modified work: 21 days With hospitalization, cognitive work: 42 days Bipolar affective disorder, depressed Rule out impaired mood/personality disorder: 0 days Without hospitalization: 0-21 days With hospitalization: 21-42 days Bipolar affective disorder, mixed Without hospitalization: 0-14 days With hospitalization: 21-42 days Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 21 Paranoia Without hospitalization: 0-14 days With hospitalization: 14-21 days Depressive type psychosis Without hospitalization: 0-56 days With hospitalization: 21-64 days Anxiety states Rule out impaired mood/personality disorder: 0 days Without hospitalization: 0-7 days With hospitalization: 14-21 days Panic disorder 1-14 days Generalized Anxiety Disorder 14-21 days Hysteria Without hospitalization: 0 days With hospitalization: 7-14 days Obsessive-compulsive disorders Without hospitalization: 0 days With hospitalization: 10 days Personality disorders 0 days Alcohol dependence syndrome Without hospitalization: 1 day Without hospitalization, considering fellow worker danger & morale: 7-14 days With hospitalization, including rehab: 14-28 days Safety sensitive position: as determined by the substance abuse professional (SAP) Acute alcoholic intoxication 1-2 days Also treated as rule violation absence Opioid type dependence Without hospitalization: 0 days Without hospitalization, considering fellow worker danger & morale: 7-14 days With hospitalization, including rehab: 14-38 days (10 days post-discharge) Safety sensitive position: as determined by the SAP Barbiturate and similarly acting sedative or hypnotic dependence Without hospitalization: 0 days Without hospitalization, considering fellow worker danger & morale: 7-14 days With hospitalization: 21 days With hospitalization, plus rehab: 28 days Safety sensitive position: as determined by the SAP 22 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Cocaine dependence Without hospitalization: 0 days Without hospitalization, considering fellow worker danger & morale: 7-14 days With hospitalization: 28 days Safety sensitive position: as determined by the SAP Cannabis dependence 0-2 days Amphetamine and other psychostimulant dependence Without hospitalization: 0 days Without hospitalization, considering fellow worker danger & morale: 7-14 days With hospitalization: 14 days With hospitalization, plus rehab: 28 days Safety sensitive position: as determined by the SAP Hallucinogen dependence Without hospitalization: 0 days Without hospitalization, considering fellow worker danger & morale: 7-14 days With hospitalization: 10 days With hospitalization, plus rehab: 28 days Safety sensitive position: as determined by the SAP Alcohol abuse 1 day Cocaine abuse Without hospitalization: 0-1 days With hospitalization: 10 days With hospitalization, plus rehab: 28 days Amphetamine or related acting sympathomimetic abuse Without hospitalization: 1 day With hospitalization: 14 days With hospitalization, plus rehab: 28 days Acute reaction to stress Without hospitalization (on-going counseling/drug therapy): 1 day With hospitalization: 10 days Unspecified acute reaction to stress, post-traumatic stress disorder Without hospitalization (on-going counseling): 1 day With hospitalization: 10 days Chemical dependence comorbidity: 28 days Adjustment Reaction Without hospitalization: 1-6 days Outpatient care: 1-6 days With inpatient hospitalization: 14-28 days Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 23 Postconcussion syndrome Mild: 1 day Severe: by report Depressive disorder, not elsewhere classified Rule out impaired mood/personality disorder: 0 days Outpatient therapy, without symptoms affecting work or other job issues: 0-7 days Outpatient therapy, with symptoms interfering with work: 21 days Outpatient therapy, with serious job satisfaction issues: 28-42 days With hospitalization, non-cognitive/modified work: 28 days With hospitalization, cognitive work: 42-56 days Attention deficit disorder 1 day (See ODG Capabilities & Activity Modifications for Restricted Work under “Work” in the Procedure Summary of the original guideline document) 8. Priority for Q-COMP Rating criteria Functional restoration Does the guideline consider graded increases in activity and function? Psychosocial factors To what degree does the guideline consider psychosocial factors that may influence recovery? Return to work process (vocational rehabilitation) To what degree does the guideline consider the Return to Work Process (vocational rehabilitation)? Risk factors for recovery To what degree does the guideline consider Risk Factors for Recovery? Total rating 24 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 3 4 4 5 16 Practice guideline for the treatment of acute stress disorders and post traumatic stress disorder Contents 1. 2. 3. 4. 5. 6. 7. Developed by ................................................................................................................................................................................... 26 Guideline status ............................................................................................................................................................................... 26 Where located/how accessed ..................................................................................................................................................... 26 Description/scope .......................................................................................................................................................................... 26 Outcomes considered .................................................................................................................................................................... 29 Agree appraisal................................................................................................................................................................................. 29 Relevance/appropriateness of use in workers’ compensation sector ............................................................................... 30 a) Functional progression ............................................................................................................................................................ 30 b) Physical/psychiatric rehabilitation ........................................................................................................................................ 33 c) Risk factor/recovery ................................................................................................................................................................ 33 d) Return to work........................................................................................................................................................................... 33 8. Priority for Q-COMP ...................................................................................................................................................................... 34 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 25 1. Developed by American Psychiatric Association. Practice guideline for the treatment of patients with acute stress disorder and post traumatic stress disorder. Arlington (VA); American Psychiatric Association: 2004 Nov. 57 p. [463 references] 2. Guideline status This is the current release of the guideline. 3. Where located/how accessed National Guideline Clearinghouse www.guideline.gov Electronic copies; Available in Portable Document Format (PDF) from the American Psychiatric Association’s Web site. Print copies; Available from the American Psychiatric Press, inc (APPI), 1400 K Street NW, Washington, DC 2005; (202) 682-6262; (800) 368-5777; fax (202) 789-2648. The following companion documents are available: • Treating patients with acute stress disorder and post traumatic stress disorder. A Quick Reference Guide. Washington, DC: APA, 2004. Electronic copies: Available in Portable Document Format (PDF) from the American Psychiatric Association (APA) Web site. • American Psychiatric Association practice guideline development process. Washington, DC: APA, 2004. Electronic copies: Available in Portable Document Format (PDF) from the APA Web site. Print copies: Available from the American Psychiatric Press, Inc (APPI), 1400 K Street NW, Washington, DC 20005; (202) 682-6262; (800) 368-5777; fax (202) 789-2648. 4. Description/scope Disease/condition(s) • Acute stress disorder and post traumatic stress disorder Guideline category • Diagnosis • Evaluation • Management • Treatment Clinical speciality • Psychiatry Intended users • Physicians Guideline objectives To assist psychiatrists in the assessment and care of adult patients with cute stress disorder (ASD) and post traumatic stress disorder (PTSD). 26 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Target population Adults (18 years of age and older) with suspected acute stress disorder or post traumatic stress disorder, according to the criteria defined in the Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition (DSM-IV). Interventions and practices considered Assessment/ Diagnosis 1. Differential diagnosis of acute stress disorder (ASD) and post traumatic stress disorder (PTSD) according to Diagnostic and Statistical Manual of Depression, 4th Edition (DSM-IV) criteria 2. History of traumatic experience 3. Complete psychiatric evaluation 4. Functional assessment 5. Determination and treatment of comorbid physical or psychiatric disorders (including major depressive disorders, anxiety disorders , and substance use disorders) 6. Determination of comorbid somatisation disorder or other somatoform disorders 7. Assessment of patients at risk for suicide 8. Assessment of patients potential to harm others Psychiatric management 1. Establishment of a therapeutic alliance with the patient 2. Patient education regarding acute stress disorder (and post traumatic stress disorder) 3. Enhancement of treatment adherence 4. Coordination of care by collaborating with other clinicians 5. Psychotherapeutic and psychoeducational interventions 6. Monitoring of patient’s treatment response 7. Monitoring for comorbid medical conditions or substance abuse disorders 8. Clinical assistance for family members who may require intervention 9. Assistance with life issues (e.g., family and social relationships, living conditions, vocational issues , and financial support) Pharmacotherapy 1. Selective serotonin reuptake inhibitors (SSRI’s) • Fluoxetine • Sertraline • Paroxetine • Fluvoxamine • Citalopram 2. Tricyclic antidepressants • Amitriptyline • Imipramine • Desipramine • Phenelzine 3. Monoamine oxidase inhibitors (MAOIs) • Phenelzine • Brofaromine • Moclobemide Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 27 4. Other antidepressants • Nefazodone • Trazodone • Bupropion • Venlafaxine • Mirtazapine 5. Second-generation antipsychotic medications • Olazapine • Quetiapine • Risperidone 6. Anticonvulscents • Divalproex • Carbamazepine • Topiramate • Lamotrigine • Tiagabine* *Note form the National Guideline Clearinghouse: On February 18, 2005, the US Food and Drug Administration (FDA) announced that a bolded Warning will be added to the labelling for Gabitril (tiagibine) to warn prescribers of the risk of seizures in patients without epilepsy being treated with this drug. Although Gabitril has been shown to reduce the frequency of seizures in patients with epilepsy, paradoxically, Gabitril’s use has been associated with the occurrence of seizures in patients without epilepsy. Gabitril is approved for use only as adjunctive therapy in adults and children 12 years and older in the treatment of partial seizures. Because Gabitril has not been systematically evaluated in adequate and well-controlled trials for any other indication, its safety and effectiveness have not been established for any other use. Cephalon will undertake an educational campaign to discourage off-label use of Gabitril. See the FDA web site for more information. 7. Other therapeutic agents • Benzodiazepines, including alprazolam • Valproic acid • Cyproheptadine • Inositil • Alpha-adrenergic blockers, including prazosin and clonidine • Bet-adrenergic blockers, including propanolol • Chloral hydrate • Lithium carbonate Psychotherapeutic Interventions 1. Cognitive behavioural therapy 2. Patient utilization of existing support network 3. Psychological debriefing 4. Single-session therapy 5. Eye movement desensitization and reprocessing (EMDR) 6. Reactive eye dilation desensitization and reprocessing (REDDR) 7. Hypnotherapy 8. Desensitization 9. Stress inoculation 28 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 10. Imagery rehearsal 11. Prolonged exposure techniques 12. Case management 13. Group therapies including present-centred and trauma-focused group therapies 14. Optimism training 15. Goal setting and achievement 16. Biofeedback 17. Multiple channel exposure therapy 18. Assertiveness training 19. Relaxation exercises 20. Internet based therapies 21. Outward Bound group recreational therapies 5. Outcomes considered • Reduction in severity of symptoms of acute stress disorder (ASD) and post traumatic disorder (PTSD) symptoms • Prevention/ reduction of trauma-related comorbid conditions • Patient adherence to treatment plan • Response to treatment • Speed of recovery • Social, occupational, adaptive, and interpersonal functioning • Length of hospitalisation • Quality of life • Rate of relapse 6. Agree appraisal • • • • • • Scope and Purpose Stakeholder Involvement Rigour of Development Clarity and Presentation Applicability Editorial Independence 67% 42% 57% 50% 0% 67% Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 29 7. Relevance/appropriateness of use in workers’ compensation sector a) Functional progression Major recommendations Each recommendation is identified as falling into one of three categories of endorsement, indicated by a bracketed Roman numeral following the statement. Definitions of the categories of endorsement are provided at the end of the “Major Recommendations” field. 1. Initial assessment The initial step in identifying individuals with acute stress disorder (ASD) or post traumatic stress disorder (PTSD) involves screening for recent or remote trauma exposure, although the clinical approach may vary depending on the recency of the traumatic event [I]. If eliciting vivid and detailed recollections of the traumatic event immediately after exposure enhances the patient’s distress, the interview may be limited to gathering information that is essential to provide needed medical care [I]. The first interventions in the aftermath of an acute trauma consist of stabilizing and supportive medical care and supportive psychiatric care and assessment [I]. After large-scale catastrophes, initial psychiatric assessment includes differential diagnosis of physical and psychological effects of the traumatic event (e.g., anxiety resulting from hemodynamic compromise, hyperventilation, somatic expressions of psychological distress, fatigue) and identification of persons or groups who are at greatest risk for subsequent psychiatric disorders, including ASD or PTSD [I]. This identification may be accomplished through individual evaluation, group interviews, consultation, and use of surveillance instruments [I]. Diagnostic evaluation may be continued after the initial period has passed and a physically and psychologically safe environment has been established, the individual’s medical condition has been stabilized, psychological reassurance has been provided, and, in disaster settings, necessary triage has been accomplished. It is important for this diagnostic assessment to include a complete psychiatric evaluation that specifically assesses for the symptoms of ASD and PTSD, including dissociative, reexperiencing, avoidance/numbing, and hyperarousal symptom clusters and their temporal sequence relative to the trauma (i.e., before versus after 1 month from the traumatic event) [I]. Other important components of the assessment process include functional assessment, determining the availability of basic care resources (e.g., safe housing, social support network, companion care, food, clothing), and identifying previous traumatic experiences and comorbid physical or psychiatric disorders, including depression and substance use disorders [I]. 2. Psychiatric management Psychiatric management for all patients with ASD or PTSD includes instituting interventions and activities to ensure physical and psychological safety, required medical care, and availability of needed resources for self-care and recovery [I]. The patient’s level of functioning and safety, including his or her risk for suicide and potential to harm others, is always important to evaluate during initial assessment and may determine the treatment setting [I]. The goals of psychiatric management for patients with ASD and PTSD also include establishing a therapeutic alliance with the patient; providing ongoing assessment of safety and psychiatric status, including possible comorbid disorders and response to treatment; and increasing the patients understanding of and active adaptive coping with psychosocial effects of exposure to the traumatic event, such as injury, job loss, or loss of loved ones [I]. Additional goals of psychiatric management include providing education regarding ASD and PTSD, enhancing treatment adherence, evaluating and managing physical health and functional impairments, and coordinating care to include collaborating with other clinicians [I]. 3. General principles of treatment selection The goals of treatment for individuals with a diagnosis of ASD or PTSD include reducing the severity of ASD or PTSD symptoms, preventing or treating trauma-related comorbid conditions that may be present or emerge, improving adaptive functioning and restoring a psychological sense of safety and trust, limiting the generalization of the danger experienced as a result of the traumatic situation(s), and protecting against relapse [I]. 30 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Patients assessed within hours or days after an acute trauma may present with overwhelming physiological and emotional symptoms (e.g., insomnia, agitation, emotional pain, dissociation). Limited clinical trial evidence is available in this area, as randomized designs are difficult to implement; however, clinical experience suggests that these acutely traumatized individuals may benefit from supportive psychotherapeutic and psychoeducational interventions [II]. Pharmacotherapy may be the first-line intervention for acutely traumatized patients whose degree of distress precludes new verbal learning or nonpharmacological treatment strategies [II]. Research has not consistently identified patient- or trauma-specific factors that predict the development of ASD or interventions that will alter the evolution of ASD into PTSD. However, early after a trauma, once the patient’s safety and medical stabilization have been addressed, supportive psychotherapy, psychoeducation, and assistance in obtaining resources such as food and shelter and locating family and friends are useful [II]. Effective treatments for the symptoms of ASD or PTSD encompass psychopharmacology, psychotherapy, and psychoeducation and other supportive measures [I]. Although studies using a combination of these approaches for ASD and PTSD are not presently available, combination treatment is widely used and may offer advantages for some patients [II]. The psychotropic medications used in clinical practice and research for the treatment of ASD and PTSD were not specifically developed for these disorders but have been used in doses similar to those recommended or approved for other psychiatric illnesses. For patients with ASD or PTSD, choice of treatment includes consideration of age and gender, presence of comorbid medical and psychiatric illnesses, and propensity for aggression or self-injurious behavior [I]. Other factors that may influence treatment choice include the recency of the precipitating traumatic event; the severity and pattern of symptoms; the presence of particularly distressing target symptoms or symptom clusters; the development of interpersonal or family issues or occupational or work-related problems; preexisting developmental or psychological vulnerabilities, including prior trauma exposure; and the patient’s preferences [I]. When the patient’s symptoms do not respond to a plan of treatment, selection of subsequent interventions will depend on clinical judgment, as there are limited data to guide the clinician. It is important to systematically review factors that may contribute to treatment nonresponse, including the specifics of the initial treatment plan and its goals and rationale, the patient’s perceptions of the effects of treatment, the patient’s understanding of and adherence to the treatment plan, and the patient’s reasons for nonadherence if nonadherence is a factor [I]. Other factors that may need to be addressed in patients who are not responding to treatment include problems in the therapeutic alliance; the presence of psychosocial or environmental difficulties; the effect of earlier life experiences such as childhood abuse or previous trauma exposures; and comorbid psychiatric disorders, including substancerelated disorders and personality disorders [I]. 4. Specific treatment strategies • Psychopharmacology Although it has been hypothesized that pharmacological treatment soon after trauma exposure may prevent the development of ASD and PTSD, existing evidence is limited and preliminary. Thus, no specific pharmacological interventions can be recommended as efficacious in preventing the development of ASD or PTSD in at-risk individuals. For patients with ASD, there are few studies of pharmacological interventions. However, selective serotonin reuptake inhibitors (SSRIs) [II] and other antidepressants [III] represent reasonable clinical interventions that are supported by limited findings in ASD as well as by findings of therapeutic benefits in patients with PTSD. SSRIs are recommended as first-line medication treatment for PTSD [I]. In both male and female patients, treatment with SSRIs has been associated with relief of core PTSD symptoms in all three symptom clusters (reexperiencing, avoidance/numbing, hyperarousal). Other antidepressants, including tricyclic antidepressants and monoamine oxidase inhibitors (MAOIs), may also be beneficial in the treatment of PTSD [II]. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 31 Benzodiazepines may be useful in reducing anxiety and improving sleep [III]. Although their efficacy in treating the core symptoms of PTSD has not been established, benzodiazepines are often used in trauma-exposed individuals and patients with PTSD. However, clinical observations include the possibility of dependence, increased incidence of PTSD after early treatment with these medications, or worsening of PTSD symptoms after withdrawal of these medications. Thus, benzodiazepines cannot be recommended as monotherapy in PTSD. In addition to being indicated in patients with comorbid psychotic disorders, second generation antipsychotic medications (e.g., olanzapine, quetiapine, risperidone) may be helpful in individual patients with PTSD [III]. Anticonvulsant medications (e.g., divalproex, carbamazepine, topiramate, lamotrigine), alpha-2- adrenergic agonists, and beta-adrenergic blockers may also be helpful in treating specific symptom clusters in individual patients [III]. • Psychotherapeutic interventions Some evidence is available about the effectiveness of psychotherapeutic intervention immediately after trauma in preventing development of ASD or PTSD. Studies of cognitive behavior therapy in motor vehicle and industrial accident survivors as well as in victims of rape and interpersonal violence suggest that cognitive behaviour therapies may speed recovery and prevent PTSD when therapy is given over a few sessions beginning 2-3 weeks after trauma exposure [II]. Early supportive interventions, psychoeducation, and case management appear to be helpful in acutely traumatized individuals, because these approaches promote engagement in ongoing care and may facilitate entry into evidence-based psychotherapeutic and psychopharmacological treatments [II]. Encouraging acutely traumatized persons to first rely on their inherent strengths, their existing support networks, and their own judgment may also reduce the need for further intervention [II]. In populations of patients who have experienced multiple recurrent traumas, there is little evidence to suggest that early supportive care delivered as a stand-alone treatment will result in lasting reductions in PTSD symptoms. However, no evidence suggests that early supportive care is harmful. In contrast, psychological debriefings or single-session techniques are not recommended, as they may increase symptoms in some settingsand appear to be ineffective in treating individuals with ASD and inpreventing PTSD. No controlled studies of psychodynamic psychotherapy, eye movement desensitization and reprocessing (EMDR), or hypnosis have been conducted that would establish data-based evidence of their efficacy as an early or preventive intervention for ASD or PTSD. For patients with a diagnosis of ASD or PTSD, available evidence and clinical experience suggest that a number of psychotherapeutic interventions may be useful. Patients with ASD may be helped by cognitive behavior therapy and other exposure-based therapies [II]. In addition, cognitive behavior therapy is an effective treatment for core symptoms of acute and chronic PTSD [I]. EMDR also appears to be effective [II]; however, therapeutic benefit for the rapid eye movement component of this therapy has not been consistently demonstrated. Stress inoculation, imagery rehearsal, and prolonged exposure techniques may also be indicated for treatment of PTSD and PTSD-associated symptoms such as anxiety and avoidance [II]. The shared element of controlled exposure of some kind may be the critical intervention. Psychodynamic psychotherapy may be useful in addressing developmental, interpersonal, or intrapersonal issues that relate to the nature, severity, symptoms, or treatment of ASD and PTSD and that may be of particular importance to social, occupational, and interpersonal functioning [II]. Case management, psychoeducation, and other supportive interventions may be useful in facilitating entry into ongoing treatment, appear not to exacerbate PTSD symptoms, and in some pilot investigations have been associated with PTSD symptom reduction [II]. Present-centered and trauma-focused group therapies may also reduce PTSD symptom severity [III]. 32 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Definitions Each recommendation is identified as falling into one of three categories of endorsement, indicated by a bracketed Roman numeral following the statement. The three categories represent varying levels of clinical confidence regarding the efficacy of the treatment for the disorder and conditions described. [I] Recommended with substantial clinical confidence [II] Recommended with moderate clinical confidence [III] May be recommended on the basis of individual circumstances. b) Physical/psychiatric rehabilitation As above. c) Risk factor/recovery Potential harms • Successful treatment may require patients to tolerate intense affect and/ordisruptive or unpleasant medication side effects. • Use of benzodiazepines may produce an increased incidence of post traumatic stress disorder (PTSD) after early treatment or worsening of PTSD symptoms after benzodiazepine withdrawal. There are also concerns about addictive potential in individuals with comorbid substance use disorders, which may prompt additional caution regarding use of benzodiazepines. • In-depth exploration of the traumatic event and the patient’s experiences may increase patient distress and result in increased symptom severity. • Insensitive or premature exploration of recent life threatening events or losses may cause the patient to avoid medical care. • Discussion of distressing memories and events in heterogeneously exposed groups may adversely affect those with little or no exposure when they hear of the frightening and terrifying experiences of others. • Psychological debriefing may increase symptoms in some patients. • Nefazodone has been associated with irreversible and life-threatening hepatic failure. Contraindications • While psychosocial treatments that attempt to identify and process traumatic experiences may be effective for individuals from Western cultures, they may be contraindicated for some Southeast Asian populations and persons from other non-Western cultures. • Clinicians reluctance to prescribe monoamine oxidase inhibitors (MAOIs) generally relates to concerns about the capacity of patients to adhere to tyramine-free diets or to abstain from alcohol, certain drugs of abuse, and contraindicated prescription medications (e.g., selective serotonin reuptake inhibitors [SSRIs], central nervous system [CNS] stimulants, decongestants, and meperidine). d) Return to work Not discussed. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 33 8. Priority for Q-COMP Rating criteria Functional restoration Does the guideline consider graded increases in activity and function? Psychosocial factors To what degree does the guideline consider psychosocial factors that may influence recovery? Return to work process (vocational rehabilitation) To what degree does the guideline consider the Return to Work Process (vocational rehabilitation)? Risk factors for recovery To what degree does the guideline consider Risk Factors for Recovery? Total rating 34 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 1 1 1 1 4 Post-traumatic stress disorder The management of PTSD in adults and children in primary and secondary care Contents 1. 2. 3. 4. 5. 6. 7. Developed by ................................................................................................................................................................................... 36 Guideline status ............................................................................................................................................................................... 36 Where located/how accessed ..................................................................................................................................................... 36 Description/scope .......................................................................................................................................................................... 36 Outcomes considered .................................................................................................................................................................... 38 Agree appraisal................................................................................................................................................................................. 38 Relevance/appropriateness of use in workers’ compensation sector ............................................................................... 39 a) Functional progression ............................................................................................................................................................ 39 b) Physical/psychiatric rehabilitation ........................................................................................................................................ 40 c) Risk factor/recovery ................................................................................................................................................................ 46 d) Return to work........................................................................................................................................................................... 46 8. Priority for Q-COMP ...................................................................................................................................................................... 46 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 35 1. Developed by National Collaborating Centre for Mental Health. Post-traumatic stress disorder: the management of PTSD in adults and children in primary and secondary care. London (UK): National Institute for Clinical Excellence (NICE);2005.167 p. [69 references] 2. Guideline status This is the current release of the guideline. 3. Where located/how accessed National Guideline Clearinghouse www.guideline.gov Electronic copies; Available in Portable Document Format [PDF] from the National Institute for Health and Clinical Excellence (NICE) Web site The following companion documents are available: • National Collaborating Centre for Mental Health. Post-traumatic stress disorder (PTSD). The management of PTSD in adults and children in primary and secondary care. NICE guideline (Clinical guideline 26). London (UK): National Institute for Health and Clinical Excellence (NICE); 2005 Mar. 41 p. Electronic copies: Available in Portable Document Format (PDF) from the National Institute for Health and Clinical Excellence (NICE) Web site. • National Collaborating Centre for Mental Health. Post-traumatic stress disorder (PTSD). The management of PTSD in adults and children in primary and secondary care. Quick reference guide. London (UK): National Institute for Health and Clinical Excellence (NICE); 2005 Mar. 17 p. Electronic copies: Available in Portable Document Format (PDF) from the NICE Web site. • Post-traumatic stress disorder--presenter slides. Available from the NICE Web site. The following patient resource is available: • Post-traumatic stress disorder (PTSD): the treatment of PTSD in adults and children. Understanding NICE guidance – information for people with PTSD, their advocates and carers, and the public. National Institute for Health and Clinical Excellence (NICE), 2005 Mar. 36 p. Available in Portable Document Format (PDF) from the National Institute for Clinical Excellence (NICE) Web site. Print copies: Available from the National Health Service (NHS) Response Line 0870 1555 455, ref N0849. 4. Description/scope Disease/condition(s) • Post-traumatic stress disorder (PTSD) Guideline category • Diagnosis • Evaluation • Management • Treatment 36 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Clinical speciality • Family Practice • Internal Medicine • Paediatrics • Psychiatry • Psychology Intended users • Intended users • Advanced Practice Nurses • Allied Health Personnel • Emergency Medical Technicians/Paramedics • Hospitals • Nurses • Occupational Therapists • Patients • Physicians • Psychologists/Non-physician Behavioural Health Clinicians • Social Workers Guideline objectives To make recommendations and suggest good practice points for the treatment and management of post-traumatic stress disorder (PTSD). Specifically, the guideline aims to: 1. 2. 3. 4. 5. Evaluate the role of specific psychological interventions in the treatment and management of PTSD Evaluate the role of specific pharmacological interventions in the treatment and management of PTSD Evaluate the role of early psychological and pharmacological interventions shortly after the traumatic event Address the issues of diagnosis, detection, and the use of screening techniques in high-risk situations Provide key review criteria for audit, which will enable objective measurements to be made of the extent and nature of local implementation of this guidance, particularly its impact upon practice and outcomes for people with PTSD. Target population Adults and children of all ages , who meet the diagnostic criteria for , or are at risk for, post-traumatic stress disorder (PTSD). Interventions and practices considered Screening and diagnosis of Post-Traumatic Stress Disorder (PTSD) 1. Symptom assessment and coordination of care (including determinations of need for emergency or psychiatric assessment) 2. Screening of individuals involved in major disasters, refugees, and asylum seekers 3. Assessment of comorbid conditions 4. Familiarisation with ethnic and cultural background of patient 5. Special considerations for assessing PTSD symptoms in children Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 37 Psychological interventions 1. Trauma focused cognitive behavioural therapy 2. Eye movement desensitisation and reprocessing (EMDR) Pharmacological therapy 1. Antidepressants • Mirtazapine 2. Selective serotonin reuptake inhibitors • Paroxetine 3. Tricyclic antidepressants • Amitriptyline 4. Monoamine oxidase inhibitors • Phenelzine 5. Hypnotic medication 6. Antipsychotic agents • Olanzapine 7. Management of side effects of therapy and discontinuation/withdrawal symptoms Other practices 1. Watchful waiting Supportive measures 1. Family and carer support 2. Disaster planning (organization of social and psychological support) Interventions considered but not recommended Serataline, fluoxetine, imipramine, venlaxafine, risperidone relaxation therapy, hypnotherapy, supportive therapy, non-directive therapy, systematic psychotherapy and psychodynamic therapy, debriefing, repetitive transcranial magnetic stimulation (rTMS). 5. Outcomes considered • • • • • Incidence and prevalence of post-traumatic stress disorder (PTSD) Symptom improvement (as measured by independent assessors or self-report) Side effects of pharmacologic therapy Relapse rate Impact on patient carers. 6. Agree appraisal • • • • • • 38 Scope and Purpose Stakeholder Involvement Rigour of Development Clarity and Presentation Applicability Editorial Independence 2% 79% 0% 2% 67% 8% Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 7. Relevance/appropriateness of use in workers’ compensation sector Recognition of Post-traumatic Stress Disorder (PTSD) Effective treatment of PTSD can only take place if the disorder is recognised. In some cases, for example following a major disaster, specific arrangements to screen people at risk may be considered. For the vast majority of people with TSD, opportunities for recognition and identification come as part of routine healthcare interventions, for example, following an assault or an accident for which physical treatment is required, or when a person discloses domestic violence or a history of childhood sexual abuse. Identification of PTSD in children presents particular problems but is improved if children are asked directly about their experiences. Recognition in primary care PTSD can present with a range of symptoms, which in most adults are most commonly in the form of very vivid, distressing memories of the event or flashbacks (otherwise known as intrusive or re-experiencing symptoms). However, at times the most prominent symptoms may be avoidance of traumarelated situations or general social contacts. It is important when recognising and identifying PTSD to ask specific questions in a sensitive manner about both the symptoms and traumatic experiences. A number of problems such as depression are often comorbid with PTSD. Often these problems will improve with the treatment of the PTSD, but where this does not happen or the comorbid disorder impedes the effective treatment of the PTSD, it may be appropriate to consider providing specific treatment for that disorder. PTSD may present with a range of symptoms (including re-experiencing, avoidance, hyperarousal, depression, emotional numbing, drug or alcohol misuse and anger) and therefore, when assessing for PTSD, members of the primary care team should ask in a sensitive manner whether or not patients with such symptoms have suffered a traumatic experience (which may have occurred many months or years before) and give specific examples of traumatic events (for example, assaults, rape, road traffic accidents, childhood sexual abuse and traumatic childbirth). General practitioners and other members of the primary care team should e aware of traumas associated with the development of PTSD. These include single events such as assaults or road traffic accidents, and domestic violence and childhood sexual abuse. For patients with unexplained physical symptoms who are repeated attendees to primary care, members of the primary care team should consider asking whether or not they have experienced a traumatic event, and provide pecific examples of traumatic events (for example, assaults, rape, road traffic accidents, childhood sexual abuse and traumatic childbirth). When seeking to identify PTSD, members of the primary care team should consider asking adults specific questions about re-experiencing (including flashbacks and nightmares) or hyperarousal (including an exaggerated startle response or sleep disturbance). For children, particularly younger children, consideration should be given to asking the child and/or the parents about sleep disturbance or significant changes in sleeping patterns. Recognition in general hospital settings Many people attending for medical services in a general hospital setting may have experienced traumatic events. This may be particularly so in emergency departments and in orthopaedic and plastic surgery clinics. For some people with PTSD, this may be the main point of contact with the healthcare system and the opportunity that this presents for the recognition and identification of PTSD should be taken. PTSD may present with a range of symptoms (including re-experiencing, avoidance, hyperarousal, depression, emotional numbing and anger) and therefore when assessing for PTSD, members of secondary care medical teams should ask in a sensitive manner whether or not patients with such symptoms have suffered a traumatic experience and give specific examples of traumatic events (for example, assaults, rape, road traffic accidents, childhood sexual abuse and traumatic childbirth). Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 39 Screening of individuals involved in a major disaster, programme refugees and asylum seekers Many individuals involved in a major disaster will suffer both short- and long-term consequences of their involvement. Although the development of single-session debriefing is not recommended, screening of all individuals should be considered by the authorities responsible for developing the local disaster plan. Similarly, the vast majority of programme refugees (people who are brought to the UK from a conflict zone through a programme organised by an agency such as the United Nations High Commission for Refugees) will have experienced major trauma and may benefit from a screening programme. For individuals at high risk of developing PTSD following a major disaster, consideration should be given (by those responsible for coordination of the disaster plan) to the routine use of a brief screening instrument for PTSD at 1 month after the disaster. For programme refugees and asylum seekers at high risk of developing PTSD, consideration should be given (by those responsible for management of the refugee programme) to the routine use of a brief screening instrument for PTSD as part of the initial refugee healthcare assessment. This should be a part of any comprehensive physical and mental health screen. Specific recognition issues for children Children, particularly those aged under 8 years, may not complain directly of PTSD symptoms such as reexperiencing or avoidance. Instead, children may complain of sleeping problems. It is therefore vital that all opportunities for identifying PTSD in children should be taken. Questioning the children as well as parents or guardians will also improve the recognition of PTSD. PTSD is common (up to 30%) in children following attendance at emergency departments for a traumatic injury. Emergency department staff should inform parents or guardians of the risk of their child developing PTSD following emergency attendance for a traumatic Injury and advise them on what action to take if symptoms develop. When assessing a child or young person for PTSD, healthcare professionals should ensure that they separately and directly question the child or young person about the presence of PTSD symptoms. They should not rely solely on information from the parent or guardian in any assessment. When a child who has been involved in a traumatic event is treated in an emergency department, emergency staff should inform the parents or guardians of the possibility of the development of PTSD, briefly describe the possible symptoms (for example, sleep disturbance, nightmares, difficulty concentrating and irritability) and suggest that they contact their general practitioner if the symptoms persist beyond 1 month. b) Physical/psychiatric rehabilitation Assessment and coordination of care For PTSD sufferers presenting in primary care, General Practitioners (GPs) should take responsibility for the initial assessment and the initial coordination of care. This includes the determination of the need for emergency medical or psychiatric assessment. Assessment of PTSD sufferers should be conducted by competent individuals and be comprehensive, including physical, psychological and social needs and a risk assessment. Patient preference should be an important determinant of the choice among effective treatments. PTSD sufferers should be given sufficient information about the nature of these treatments to make an informed choice. Where management is shared between primary and secondary care, there should be clear agreement among individual healthcare professionals about the responsibility for monitoring patients with PTSD. This agreement should be in writing (where appropriate, using the Care Programme Approach) and should be shared with the patient and, where appropriate, their family and carers. 40 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Support for families and carers Families and carers have a central role in supporting people with PTSD. However, depending on the nature of the trauma and its consequences, many families may also need support for themselves. Healthcare professionals should be aware of the impact of PTSD on the whole family. In all cases of PTSD, healthcare professionals should consider the impact of the traumatic event on all family members and, when appropriate, assess this impact and consider providing appropriate support. Healthcare professionals should ensure, where appropriate and with the consent of the PTSD sufferer where necessary, that the families of PTSD sufferers are fully informed about common reactions to traumatic events, including the symptoms of PTSD and its course and treatment. In addition to the provision of information, families and carers should be informed of self-help groups and support groups and encouraged to participate in such groups where they exist. When a family is affected by a traumatic event, more than one family member may suffer from PTSD. If this is the case, healthcare professionals should ensure that the treatment of all family members is effectively coordinated. Practical support and social factors Practical and social support can play an important part in facilitating a person’s recovery from PTSD, particularly immediately after the trauma. Healthcare professionals should be aware of this and advocate for such support when people present with PTSD. Healthcare professionals should identify the need for appropriate information about the range of emotional responses that may develop and provide practical advice on how to access appropriate services for these problems. They should also identify the need for social support and advocate the meeting of this need. Healthcare professionals should consider offering help or advice to PTSD sufferers or relevant others on how continuing threats related to the traumatic event may be alleviated or removed. Language and culture People with PTSD treated in the National Health Service (NHS) come from diverse cultural and ethnic backgrounds and some have no or limited English, but all should be offered the opportunity to benefit from psychological interventions. This can be achieved by the use of interpreters and bicultural therapists. In all cases, healthcare professionals must familiarise themselves with the cultural background of the sufferer. Where a PTSD sufferer has a different cultural or ethnic background from that of the healthcare professionals who are providing care, the healthcare professionals should familiarise themselves with the cultural background of the PTSD sufferer. Where differences of language or culture exist between healthcare professionals and PTSD sufferers, this should not be an obstacle to the provision of effective trauma-focused psychological interventions. Where language or culture differences present challenges to the use of trauma-focused psychological interventions in PTSD, healthcare professionals should consider the use of interpreters and bicultural therapists. Healthcare professionals should pay particular attention to the identification of individuals with PTSD where the culture of the working or living environment is resistant to recognition of the psychological consequences of trauma. Care for all people with PTSD PTSD responds to a variety of effective treatments. All treatment should be supported by appropriate information to sufferers about the likely course of such treatment. A number of factors, which are described below, may modify the nature, timing and course of treatment. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 41 Care across all conditions When developing and agreeing a treatment plan with a PTSD sufferer, healthcare professionals should ensure that sufferers receive information about common reactions to traumatic events, including the symptoms of PTSD and its course and treatment. Healthcare professionals should not delay or withhold treatment for PTSD because of court proceedings or applications for compensation. Healthcare professionals should be aware that many PTSD sufferers are anxious about and can avoid engaging in treatment. Healthcare professionals should also recognize the challenges that this presents and respond appropriately, for example by following up PTSD sufferers who miss scheduled appointments. Healthcare professionals should treat PTSD sufferers with respect, trust and understanding, and keep technical language to a minimum. Healthcare professionals should normally only consider providing traumafocused psychological treatment when the sufferer considers it safe to proceed. Treatment should be delivered by competent individuals who have received appropriate training. These individuals should receive appropriate supervision. Comorbidities When a patient presents with PTSD and depression, healthcare professionals should consider treating the PTSD first, as the depression will often improve with successful treatment of the PTSD. For PTSD sufferers whose assessment identifies a high risk of suicide or harm to others, healthcare professionals should first concentrate on management of this risk. For PTSD sufferers who are so severely depressed that this makes initial psychological treatment of PTSD very difficult (for example, as evidenced by extreme lack of energy and concentration, inactivity, or high suicide risk), healthcare professionals should treat the depression first. For PTSD sufferers with drug or alcohol dependence or in whom alcohol or drug use may significantly interfere with effective treatment, healthcare professionals should treat the drug or alcohol problem first. When offering trauma-focused psychological interventions to PTSD sufferers with comorbid personality disorder, healthcare professionals should consider extending the duration of treatment. People who have lost a close friend or relative due to an unnatural or sudden death should be assessed for PTSD and traumatic grief. In most cases, healthcare professionals should treat the PTSD first without avoiding discussion of the grief. Treatment of PTSD Early interventions A number of sufferers with PTSD may recover with no or limited interventions. However, without effective treatment, many people may develop chronic problems over many years. The severity of the initial traumatic response is a reasonable indicator of the need for early intervention, and treatment should not be withheld in such circumstances. Watchful Waiting Where symptoms are mild and have been present for less than 4 weeks after the trauma, watchful waiting, as a way of managing the difficulties presented by individual sufferers, should be considered by healthcare professionals. A follow-up contact should be arranged within 1 month. 42 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Immediate Psychological Interventions for All As described in this guideline, practical support delivered in an empathetic manner is important in promoting recovery for PTSD, but it is unlikely that a single session of a psychological intervention will be helpful. All health and social care workers should be aware of the psychological impact of traumatic incidents in their immediate post-incident care of survivors and offer practical, social and emotional support to those involved. For individuals who have experienced a traumatic event, the systematic provision to that individual alone of brief, single-session interventions (often referred to as debriefing) that focus on the traumatic incident should not be routine practice when delivering services. PTSD where symptoms are present within 3 months of a trauma Brief psychological interventions (five sessions) may be effective if treatment starts within the first month after the traumatic event. Beyond the first month, the duration of treatment is similar to that for chronic PTSD. Trauma-focused cognitive-behavioural therapy should be offered to those with severe post-traumatic symptoms or with severe PTSD in the first month after the traumatic event. These treatments should normally be provided on an individual out-patient basis. Trauma-focused CBT should be offered to people who present with PTSD within 3 months of a traumatic event. The duration of the trauma-focused CBT should normally be 8-12 sessions, but if the treatment starts in the first month after the event, fewer sessions (about 5) may be sufficient. When the trauma is discussed in the treatment session, longer sessions (for example, 90 min) are usually necessary. Treatment should be regular and continuous (usually at least once a week) and should be delivered by the same person. Drug treatment may be considered in the acute phase of PTSD for the management of sleep disturbance. In this case, hypnotic medication may be appropriate for short-term use but, if longer-term drug treatment is required, consideration should also be given to the use of suitable antidepressants at an early stage in order to reduce the later risk of dependence. Non-trauma-focused interventions such as relaxation or non-directive therapy, which do not address traumatic memories, should not routinely be offered to people who present with PTSD symptoms within 3 months of a traumatic event. PTSD where symptoms have been present for more than 3 months after a trauma Most patients presenting with PTSD have had the problem for many months, if not years. The interventions outlined below are effective in treating such individuals and duration of the disorder does not itself seem an impediment to benefiting from effective treatment provided by competent healthcare professionals. Psychological Interventions All PTSD sufferers should be offered a course of trauma-focused psychological treatment (trauma-focused CBT or eye movement desensitisation and reprocessing). These treatments should normally be provided on an individual out-patient basis. Trauma-focused psychological treatment should be offered to PTSD sufferers regardless of the time that has elapsed since the trauma. The duration of trauma-focused psychological treatment should normally be 8- 12 sessions when the PTSD results from a single event. When the trauma is discussed in the treatment session, longer sessions than usual are generally necessary (for example, 90 min). Treatment should be regular and continuous (usually at least once a week) and should be delivered by the same person. Healthcare professionals should consider extending the duration of treatment beyond 12 sessions if several problems need to be addressed in the treatment of PTSD sufferers, particularly after multiple traumatic events, traumatic bereavement or where chronic disability resulting from the trauma, significant comorbid disorders or Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 43 social problems are present. Trauma-focused treatment needs to be integrated into an overall plan of care. For some PTSD sufferers it may initially be very difficult and overwhelming to disclose details of their traumatic events. In these cases, healthcare professionals should consider devoting several sessions to establishing a trusting therapeutic relationship and emotional stabilisation before addressing the traumatic event. Non-trauma-focused interventions such as relaxation or non-directive therapy, which do not address traumatic memories, should not routinely be offered to people who present with chronic PTSD. For PTSD sufferers who have no or only limited improvement with a specific trauma-focused psychological treatment, healthcare professionals should consider the following options: • an alternative form of trauma-focused psychological treatment • the augmentation of trauma-focused psychological treatment with a course of pharmacological treatment. When PTSD sufferers request other forms of psychological treatment (for example, supportive therapy/nondirective therapy, hypnotherapy, psychodynamic therapy or systemic psychotherapy), they should be informed that there is as yet no convincing evidence for a clinically important effect of these treatments on PTSD. Drug treatment The evidence base for drug treatments in PTSD is limited. There is evidence of clinically significant benefits for mirtazapine, amitriptyline and phenelzine. (Dietary guidance is required with phenelzine.) For paroxetine there were statistically but not clinically significant benefits on the main outcome variables. Nevertheless, this drug has also been included in the list of recommended drugs. This is the only drug in the list of recommendations with a current UK product licence for PTSD. Drug treatments for PTSD should not be used as a routine first-line treatment for adults (in general use or by specialist mental health professionals) in preference to a trauma-focused psychological therapy. Drug treatments (paroxetine or mirtazapine for general use, and amitriptyline or phenelzine for initiation only by mental health specialists) should be considered for the treatment of PTSD in adults where a sufferer expresses a preference not to engage in a trauma-focused psychological treatment. Drug treatments (paroxetine or mirtazapine for general use, and amitriptyline or phenelzine for initiation only by mental health specialists) should be offered to adult PTSD sufferers who cannot start a psychological therapy because of serious ongoing threat of further trauma (for example, where there is ongoing domestic violence). Drug treatments (paroxetine or mirtazapine for general use and amitriptyline or phenelzine for initiation only by mental health specialists) should be considered for adult PTSD sufferers who have gained little or no benefit from a course of trauma-focused psychological treatment. Where sleep is a major problem for an adult PTSD sufferer, hypnotic medication may be appropriate for short-term use but, if longer-term drug treatment is required, consideration should also be given to the use of suitable antidepressants at an early stage in order to reduce the later risk of dependence. Drug treatments (paroxetine or mirtazapine for general use and amitriptyline or phenelzine for initiation only by mental health specialists) for PTSD should be considered as an adjunct to psychological treatment in adults where there is significant comorbid depression or severe hyperarousal that significantly impacts on a sufferer’s ability to benefit from psychological treatment. When an adult sufferer with PTSD has not responded to a drug treatment, consideration should be given to increasing the dosage within approved limits. If further drug treatment is considered, this should generally be with a different class of antidepressant or involve the use of adjunctive olanzapine. When an adult sufferer with PTSD has responded to drug treatment, it should be continued for at least 12 months before gradual withdrawal. 44 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions General Recommendations Regarding Drug Treatment All PTSD sufferers who are prescribed antidepressants should be informed, at the time that treatment is initiated, of potential side-effects and discontinuation/withdrawal symptoms (particularly with paroxetine). Adult PTSD sufferers started on antidepressants who are considered to have an increased suicide risk and all patients aged between 18 and 29 years (because of the potential increased risk of suicidal thoughts associated with the use of antidepressants in this age group) should normally be seen after 1 week and frequently thereafter until the risk is no longer considered significant. Particularly in the initial stages of SSRI treatment, practitioners should actively seek out signs of akathisia, suicidal ideation and increased anxiety and agitation. They should also advise PTSD sufferers of the risk of these symptoms in the early stages of treatment and advise them to seek help promptly if these are at all distressing. If a PTSD sufferer develops marked and/or prolonged akathisia while taking an antidepressant, the use of the drug should be reviewed. Adult PTSD sufferers started on antidepressants who are not considered to be at increased risk of suicide should normally be seen after 2 weeks and thereafter on an appropriate and regular basis, for example, at intervals of 2-4 weeks in the first 3 months, and at greater intervals thereafter, if response is good. Recommendations Regarding Discontinuation/Withdrawal Symptoms Discontinuation/withdrawal symptoms are usually mild and self-limiting but occasionally can be severe. Prescribers should normally gradually reduce the dosage of antidepressants over a 4-week period, although some people may require longer periods. If discontinuation/withdrawal symptoms are mild, practitioners should reassure the PTSD sufferer and arrange for monitoring. If symptoms are severe, the practitioner should consider reintroducing the original antidepressant (or another with a longer half-life from the same class) and reduce gradually while monitoring symptoms. Chronic disease management Chronic disease management models should be considered for the management of people with chronic PTSD who have not benefited from a number of courses of evidence-based treatment. Children It is particularly difficult to identify PTSD in children (see section above titled “Specific Recognition Issues for Children”). The treatments for children with PTSD are less developed but emerging evidence provides an indication for effective interventions. Early Intervention Trauma-focused CBT should be offered to older children with severe post traumatic symptoms or with severe PTSD in the first month after the traumatic event. PTSD Where Symptoms Have Been Present for More Than 3 Months After a Trauma Children and young people with PTSD, including those who have been sexually abused, should be offered a course of trauma-focused CBT adapted appropriately to suit their age, circumstances and level of development. The duration of trauma-focused psychological treatment for children and young people with chronic PTSD should normally be 8–12 sessions when the PTSD results from a single event. When the trauma is discussed in the treatment session, longer sessions than usual are usually necessary (for example, 90 min). Treatment should be regular and continuous (usually at least once a week) and should be delivered by the same person. Drug treatments should not be routinely prescribed for children and young people with PTSD. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 45 Where appropriate, families should be involved in the treatment of PTSD in children and young people. However, treatment programmes for PTSD in children and young people that consist of parental involvement alone are unlikely to be of any benefit for PTSD symptoms. When considering treatments for PTSD, parents and, where appropriate, children and young people should be informed that, apart from trauma-focused psychological interventions, there is at present no good evidence for the efficacy of widely used forms of treatment of PTSD such as play therapy, art therapy or family therapy. Disaster planning Both health and social services have a role in organising the appropriate social and psychological support for those affected by disasters. Disaster plans should include provision for a fully coordinated psychosocial response to the disaster. Those responsible for developing the psychosocial aspect of a disaster plan should ensure it contains the following: provision for immediate practical help, means to support the affected communities in caring for those involved in the disaster and the provision of specialist mental health, evidence based assessment and treatment services. All healthcare workers involved in a disaster plan should have clear roles and responsibilities, which should be agreed in advance. c) Risk factor/recovery Potential harms • Side effects of paroxetine may include anxiety, agitation, suicidal thoughts and akathisia. • Dietary restrictions and careful monitoring are required for patients taking monoamine oxidase inhibitors. • Medication discontinuation/withdrawal symptoms may occur. • Administration of some drugs to nursing mothers may lead to effects in breastfeeding infants. d) Return to work Not discussed. 8. Priority for Q-COMP Rating criteria Functional restoration Does the guideline consider graded increases in activity and function? Psychosocial factors To what degree does the guideline consider psychosocial factors that may influence recovery? Return to work process (vocational rehabilitation) To what degree does the guideline consider the Return to Work Process (vocational rehabilitation)? Risk factors for recovery To what degree does the guideline consider Risk Factors for Recovery? Total rating 46 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 1 3 0 3 7 Anxiety: Management of anxiety (panic disorder, with or without agoraphobia, and generalised anxiety disorder) in adults in primary secondary and community care Contents 1. 2. 3. 4. 5. 6. 7. Developed by ................................................................................................................................................................................... 48 Guideline status ............................................................................................................................................................................... 48 Where located/how accessed ..................................................................................................................................................... 48 Description/scope .......................................................................................................................................................................... 48 Outcomes considered .................................................................................................................................................................... 49 Agree appraisal................................................................................................................................................................................. 49 Relevance/appropriateness of use in workers’ compensation sector ............................................................................... 49 a) Functional progression ............................................................................................................................................................ 49 b) Physical/psychiatric rehabilitation ........................................................................................................................................ 50 c) Risk factor/recovery ................................................................................................................................................................ 64 d) Return to work........................................................................................................................................................................... 64 8. Priority for Q-COMP ...................................................................................................................................................................... 65 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 47 1. Developed by National Collaborating Centre for Primary Care. 2. Guideline status Current published December 2004. 3. Where located/how accessed NICE website (www.nice.org.uk/CGO22NICEguideline) An abridged version of this guidance is also available from the same site. Printed copies of the quick reference guide can be obtained from the NHS Response Line: telephone 0870 1555 455 and quote reference number N0763. Information for the Public is available from the NICE website or from the NHS Response Line (quote reference number N0764 for a version in English and N0765 for a version in English and Welsh). 4. Description/scope Disease/condition(s) Anxiety disorders including: 1. 2. 3. 4. 5. 6. 7. 8. 9. Panic disorder without agoraphobia Panic disorder with agoraphobia Specific phobia Social anxiety disorder (SAD)/Social phobia Generalised anxiety disorder (GAD) Obsessive compulsive disorder (OCD) Post traumatic stress disorder (PTSD) Acute stress disorder Adjustment disorder with anxiety Guideline category • None stated Clinical speciality • None stated Intended users • Primary health care physicians Guideline objectives The guidelines are developed in an attempt to provide optimal care and good outcomes to patients with anxiety disorders. In particular it aims to assist primary health care physicians in clinical decision making when assessing and treating patients with anxiety. 48 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Target population None stated. Interventions and Practices Considered Interventions and Practices Considered 1. 2. 3. 4. 5. 6. 7. 8. 9. Clinical evaluation of anxiety disorders Treatment settings for anxiety disorders Psychosocial interventions for anxiety disorders Treatments for different types of anxiety disorders Psychosocial interventions Medications for anxiety disorders Choosing and combining medical and psychological interventions Anxiety and co-exiting conditions Long-term treatment 5. Outcomes considered The overall aim of the treatment is to control and remove symptoms, reduce morbidity and improve overall functioning. 6. Agree appraisal • • • • • • Scope and Purpose Stakeholder Involvement Rigour of Development Clarity and Presentation Applicability Editorial Independence 72% 79% 48% 83% 44% 42% 7. Relevance/appropriateness of use in workers’ compensation sector a) Functional progression Functional progression is not specifically stated. Clinical Algorithms are provided in the full version of the original guideline document for: • Management of panic disorder in primary care: Steps 2-4 • Management of generalised anxiety disorder in primary care: Steps 2-4 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 49 b) Physical/psychiatric rehabilitation Rehabilitation is not specifically stated. The guideline covers general management, stepped approach to care, psychological interventions, pharmacological interventions, self-help interventions, monitoring and follow up. Major recommendations Diagnosis and decision making Recognition and diagnosis of panic disorder and generalised anxiety disorder Consultation Skills All healthcare professionals involved in diagnosis and management should have a demonstrably high standard of consultation skills so that a structured approach can be taken to the diagnosis and subsequent management plan for panic disorder and generalised anxiety disorder. The standards detailed in the video workbook Summative Assessment For General Practice Training: Assessment Of Consulting Skills - the Member of the Royal College of General Practitioners (MRCGP)/Summative Assessment Single Route (see www.rcgp.org.uk/exam) and required of the Membership of the Royal College of General Practitioners are a good example of standards for consulting skills. Diagnosis The accurate diagnosis of panic disorder or generalised anxiety disorder is central to the effective management of these conditions. It is acknowledged that frequently there are other conditions present, such as depression, that can make the presentation and diagnosis confusing. An algorithm has been developed to aid the clinician in the diagnostic process, and to identify which guideline is most appropriate to support the clinician in the management of the individual patient. The diagnostic process should elicit necessary relevant information such as personal history, any self medication, and cultural or other individual characteristics that may be important considerations in subsequent care. There is insufficient evidence on which to recommend a well-validated, self-reporting screening instrument to use in the diagnostic process, and so consultation skills should be relied upon to elicit all necessary information. Comorbidities The clinician should be alert to the common clinical situation of comorbidity, in particular, anxiety with depression and anxiety with substance abuse. The main problem(s) to be treated should be identified through a process of discussion with the patient. In determining the priorities of the comorbidities, the sequencing of the problems should be clarified. This can be helped by drawing up a timeline to identify when the various problems developed. By understanding when the symptoms developed, a better understanding of the relative priorities of the comorbidities can be achieved, and there is a better opportunity of developing an effective intervention that fits the needs of the individual. When the patient has depression or anxiety with depression, the National Institute for Health and Clinical Excellence (NICE) guideline on management of depression should be followed. Presentation in Accident and Emergency (A&E) with Panic Attacks It is important to remember that a panic attack does not necessarily constitute a panic disorder, and appropriate treatment of a panic attack may limit the development of panic disorder. For people who present with chest pain at A&E services, there appears to be a greater likelihood of the cause being panic disorder if coronary artery disease is not present or the patient is female or relatively young. Two other variables, atypical chest pain and self-reported anxiety, may also be associated with panic disorder presentations, but there is insufficient evidence to establish a relationship. 50 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions If a patient presents in A&E, or other settings, with a panic attack, they should: • • • • • • Be asked if they are already receiving treatment for panic disorder Undergo the minimum investigations necessary to exclude acute physical problems Not usually be admitted to a medical or psychiatric bed Be referred to primary care for subsequent care, even if assessment has been undertaken in A&E Be given appropriate written information about panic attacks and why they are being referred to primary care Be offered appropriate written information about sources of support, including local and national voluntary and self-help groups. Shared Decision-Making and Information Provision People who have panic disorder or generalised anxiety disorder and their carers need comprehensive information, presented in clear and understandable language, about the nature of their condition and the treatment options available. Such information is essential for shared decision-making between patients and healthcare professionals, particularly when making choices between broadly equivalent treatments. In addition, given the emotional, social, and economic costs that generalised anxiety disorder or panic disorder usually entail, patients and their families may need help in contacting support and self-help groups. Support groups can also promote understanding and collaboration between patients, their carers, and healthcare professionals at all levels of primary and secondary care. Shared decision-making should take place as it improves concordance and clinical outcomes. Shared decision-making between the individual and healthcare professionals should take place during the process of diagnosis and in all phases of care. Patients and, when appropriate, families and carers should be provided with information on the nature, course, and treatment of panic disorder or generalised anxiety disorder, including information on the use and likely side-effect profile of medication. To facilitate shared decision-making, evidence-based information about treatments should be available and discussion of the possible options should take place. Patient preference and the experience and outcome of previous treatment(s) should be considered in determining the choice of treatment. Common concerns about taking medication, such as fears of addiction, should be addressed. In addition to being provided with high-quality information, patients, families, and carers should be informed of self-help groups and support groups and be encouraged to participate in such programmes where appropriate. Language When talking to patients and carers, healthcare professionals should use everyday, jargon free language. If technical terms are used, they should be explained to the patient. Where appropriate, all services should provide written material in the language of the patient, and appropriate interpreters should be sought for people whose preferred language is not English. Where available, consideration should be given to providing psychotherapies in the patient’s own language if this is not English. Screening tools There is insufficient evidence on which to recommend a well-validated, self-reporting screening instrument to use in the diagnostic process, and so consultation skills should be relied upon to elicit all necessary information. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 51 Care of people with panic disorder Step 1: Recognition and diagnosis of panic disorder (see above) Step 2: Offer treatment in primary care The recommended treatment options have an evidence base: psychological therapy, medication, and self-help have all been shown to be effective. The choice of treatment will be a consequence of the assessment process and shared decision-making. There may be instances when the most effective intervention is not available (for example, cognitive behavioural therapy [CBT]) or is not the treatment option chosen by the patient. In these cases, the healthcare professional will need to consider, after discussion with the patient, whether it is acceptable to offer one of the other recommended treatments. If the preferred treatment option is currently unavailable, the healthcare professional will also have to consider whether it is likely to become available within a useful timeframe. Benzodiazepines are associated with a less good outcome in the long term and should not be prescribed for the treatment of individuals with panic disorder. Sedating antihistamines or antipsychotics should not be prescribed for the treatment of panic disorder. In the care of individuals with panic disorder, any of the following types of intervention should be offered and the preference of the person should be taken into account. The interventions that have evidence for the longest duration of effect, in descending order are: • Psychological therapy • Pharmacological therapy (antidepressant medication) • Self-help The treatment option of choice should be available promptly. There are positive advantages of services based in primary care (for example, lower rates of people who do not attend) and these services are often preferred by patients. Psychological Interventions Cognitive behavioural therapy (CBT) should be used. CBT should be delivered only by suitably trained and supervised people who can demonstrate that they adhere closely to empirically grounded treatment protocols. CBT in the optimal range of duration (7-14 hours in total) should be offered. For most people, CBT should take the form of weekly sessions of 1-2 hours and should be completed within a maximum of 4 months of commencement. Briefer CBT should be supplemented with appropriate focussed information and tasks. Where briefer CBT is used, it should be around 7 hours and designed to integrate with structured self-help materials. For a few people, more intensive CBT over a very short period of time might be appropriate. 52 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Pharmacological Interventions The following must be taken into account when deciding which medication to offer: • The age of the patient • Previous treatment response • Risks • The likelihood of accidental overdose by the person being treated and by other family members if appropriate • The likelihood of deliberate self-harm, by overdose or otherwise • Tolerability • The preference of the person being treated • Cost, where equal effectiveness is demonstrated All patients who are prescribed antidepressants should be informed, at the time that treatment is initiated, of potential side effects (including transient increase in anxiety at the start of treatment) and of the risk of discontinuation/withdrawal symptoms if the treatment is stopped abruptly or in some instances if a dose is missed or, occasionally, on reducing the dose of the drug. Patients started on antidepressants should be informed about the delay in onset of effect, the time course of treatment, the need to take medication as prescribed, and possible discontinuation/withdrawal symptoms. Written information appropriate to the patient’s needs should be made available. Unless otherwise indicated, a selective serotonin reuptake inhibitor (SSRI) licensed for panic disorder should be offered. If an SSRI is not suitable or there is no improvement after a 12-week course and if a further medication is appropriate, imipramine or clomipramine (which are not licensed for panic disorder but have been shown to be effective in its management) may be considered. When prescribing an antidepressant, the healthcare professional should consider the following: Side effects on the initiation of antidepressants may be minimised by starting at a low dose and increasing the dose slowly until a satisfactory therapeutic response is achieved. In some instances, doses at the upper end of the indicated dose range may be necessary and should be offered if needed. Long-term treatment may be necessary for some people and should be offered if needed. If the patient is showing improvement on treatment with an antidepressant, the medication should be continued for at least 6 months after the optimal dose is reached, after which the dose can be tapered. If there is no improvement after a 12-week course, an antidepressant from the alternative class (if another medication is appropriate) or another form of therapy should be offered. Patients should be advised to take their medication as prescribed. This may be particularly important with short half-life medication in order to avoid discontinuation/withdrawal symptoms. Stopping antidepressants abruptly can cause discontinuation/withdrawal symptoms. To minimise the risk of discontinuation/withdrawal symptoms when stopping antidepressants, the dose should be reduced gradually over an extended period of time. All patients prescribed antidepressants should be informed that, although the drugs are not associated with tolerance and craving, discontinuation/withdrawal symptoms may occur on stopping or missing doses or, occasionally, on reducing the dose of the drug. These symptoms are usually mild and self-limiting but occasionally can be severe, particularly if the drug is stopped abruptly. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 53 Healthcare professionals should inform patients that the most commonly experienced discontinuation/withdrawal symptoms are dizziness, numbness and tingling, gastrointestinal disturbances (particularly nausea and vomiting), headache, sweating, anxiety, and sleep disturbances. Healthcare professionals should inform patients that they should seek advice from their medical practitioner if they experience significant discontinuation/withdrawal symptoms. If discontinuation/withdrawal symptoms are mild, the practitioner should reassure the patient and monitor symptoms. If severe symptoms are experienced after discontinuing an antidepressant, the practitioner should consider reintroducing it (or prescribing another from the same class that has a longer half-life) and gradually reducing the dose while monitoring symptoms. Self-help Bibliotherapy based on CBT principles should be offered. Information about support groups, where they are available, should be offered. (Support groups may provide face-to-face meetings, telephone conference support groups [which can be based on CBT principles], or additional information on all aspects of anxiety disorders plus other sources of help.) The benefits of exercise as part of good general health should be discussed with all patients as appropriate. NICE 2002 – Current research suggests that the delivery of cognitive behavioural therapy via a computer interface (CCBT) may be of value in the management of anxiety and depressive disorders. This evidence is, however, an insufficient basis on which to recommend the general introduction of this technology into the National Health Service (NHS). Step 3: Review and offer alternative treatment if appropriate If, after a course of treatment, the clinician and patient agree that there has been no improvement with one type of intervention, the patient should be reassessed and consideration given to trying one of the other types of intervention. Step 4: Review and offer referral from primary care if appropriate In most instances, if there have been two interventions provided (any combination of psychological intervention, medication, or bibliotherapy) and the person still has significant symptoms, then referral to specialist mental health services should be offered. Step 5: Care in specialist mental health services Specialist mental health services should conduct a thorough, holistic re-assessment of the individual, their environment, and social circumstances. This reassessment should include evaluation of: • • • • • • • Previous treatments, including effectiveness and concordance Any substance use, including nicotine, alcohol, caffeine, and recreational drugs Comorbidities Day-to-day functioning Social networks Continuing chronic stressors The role of agoraphobic and other avoidant symptoms A comprehensive risk assessment should be undertaken and an appropriate risk management plan developed. To undertake these evaluations and to develop and share a full formulation, more than one session may be required and should be available. 54 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Care and management should be based on the individual’s circumstances and shared decisions made. Options include: • Treatment of comorbid conditions • CBT with an experienced therapist if not offered already, including home based CBT if attendance at clinic is difficult • Structured problem solving • Full exploration of pharmaco-therapy • Day support to relieve carers and family members • Referral for advice, assessment or management to tertiary centres There should be accurate and effective communication between all healthcare professionals involved in the care of any person with panic disorder, and particularly between primary care clinicians (General Practitioner [GP] and teams) and secondary care clinicians (community mental health teams) if there are existing physical health conditions that also require active management. Monitoring and follow up Psychological Interventions There should be a process within each practice to assess the progress of a person undergoing CBT. The nature of that process should be determined on a case-by-case basis. Pharmacological Interventions When a new medication is started, the efficacy and side-effects should be reviewed within 2 weeks of starting treatment and again at 4, 6, and 12 weeks. Follow the Summary of Product Characteristics (SPC) with respect to all other monitoring required. At the end of 12 weeks an assessment of the effectiveness of the treatment should be made and a decision made as to whether to continue or consider an alternative intervention. If medication is to be continued beyond 12 weeks, the individual should be reviewed at 8- to 12-week intervals, depending on clinical progress and individual circumstances. Self-Help Interventions Individuals receiving self-help interventions should be offered contact with primary healthcare professionals, so that progress can be monitored and alternative interventions considered if appropriate. The frequency of such contact should be determined on a case-by-case basis, but is likely to be between every 4 and 8 weeks. Outcome Measures Short, self-complete questionnaires (such as the panic subscale of the agoraphobic mobility inventory for individuals with panic disorder) should be used to monitor outcomes wherever possible. Interventions for panic disorder Pharmacological compared with psychological compared with combination interventions for panic disorder In the care of individuals with panic disorder, any of the following types of intervention should be offered and the preference of the person should be taken into account. The interventions that have evidence for the longest duration of effect, in descending order are: • Psychological therapy • Pharmacological therapy (antidepressant medication) • Self-help Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 55 The treatment option of choice should be available promptly. There are positive advantages of services based in primary care (for example, lower rates of people who do not attend) and these services are often preferred by patients. Pharmacological interventions for panic disorder Benzodiazepines are associated with a less good outcome in the long term and should not be prescribed for the treatment of individuals with panic disorder. Sedating antihistamines or antipsychotics should not be prescribed for the treatment of panic disorder. The following must be taken into account when deciding which medication to offer: • • • • • • • • The age of the patient Previous treatment response Risks The likelihood of accidental overdose by the person being treated and by other family members if appropriate The likelihood of deliberate self-harm, by overdose or otherwise Tolerability The preference of the person being treated Cost, where equal effectiveness is demonstrated All patients who are prescribed antidepressants should be informed, at the time that treatment is initiated, of potential side effects (including transient increase in anxiety at the start of treatment) and of the risk of discontinuation/withdrawal symptoms if the treatment is stopped abruptly or in some instances if a dose is missed or, occasionally, on reducing the dose of the drug. Patients started on antidepressants should be informed about the delay in onset of effect, the time course of treatment, the need to take medication as prescribed, and possible discontinuation/withdrawal symptoms. Written information appropriate to the patient’s needs should be made available. Unless otherwise indicated, an SSRI licensed for panic disorder should be offered. If an SSRI is not suitable or there is no improvement after a 12-week course and if a further medication is appropriate, imipramine or clomipramine (which are not licensed for panic disorder but have been shown to be effective in its management) may be considered. When prescribing an antidepressant, the healthcare professional should consider the following: Side effects on the initiation of antidepressants may be minimised by starting at a low dose and increasing the dose slowly until a satisfactory therapeutic response is achieved. In some instances, doses at the upper end of the indicated dose range may be necessary and should be offered if needed. Long-term treatment may be necessary for some people and should be offered if needed. If the patient is showing improvement on treatment with an antidepressant, the medication should be continued for at least 6 months after the optimal dose is reached, after which the dose can be tapered. If there is no improvement after a 12-week course, an antidepressant from the alternative class (if another medication is appropriate) or another form of therapy should be offered. Patients should be advised to take their medication as prescribed. This may be particularly important with short half-life medication in order to avoid discontinuation/withdrawal symptoms. 56 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Stopping antidepressants abruptly can cause discontinuation/withdrawal symptoms. To minimise the risk of discontinuation/withdrawal symptoms when stopping antidepressants, the dose should be reduced gradually over an extended period of All patients prescribed antidepressants should be informed that, although the drugs are not associated with tolerance and craving, discontinuation/withdrawal symptoms may occur on stopping or missing doses or, occasionally, on reducing the dose of the drug. These symptoms are usually mild and self-limiting but occasionally can be severe, particularly if the drug is stopped abruptly. Healthcare professionals should inform patients that the most commonly experienced discontinuation/withdrawal symptoms are dizziness, numbness and tingling, gastrointestinal disturbances (particularly nausea and vomiting), headache, sweating, anxiety, and sleep disturbances. Healthcare professionals should inform patients that they should seek advice from their medical practitioner if they experience significant discontinuation/withdrawal symptoms. If discontinuation/withdrawal symptoms are mild, the practitioner should reassure the patient and monitor symptoms. If severe symptoms are experienced after discontinuing an antidepressant, the practitioner should consider reintroducing it (or prescribing another from the same class that has a longer half-life) and gradually reducing the dose while monitoring symptoms. Psychological interventions for panic disorder CBT should be used. CBT should be delivered only by suitably trained and supervised people who can demonstrate that they adhere closely to empirically grounded treatment protocols. CBT in the optimal range of duration (7-14 hours in total) should be offered. For most people, CBT should take the form of weekly sessions of 1-2 hours and should be completed within a maximum of 4 months of commencement. Briefer CBT should be supplemented with appropriate focussed information and tasks. Where briefer CBT is used, it should be around 7 hours and designed to integrate with structured self-help materials. For a few people, more intensive CBT over a very short period of time might be appropriate. Other interventions for panic disorder Bibliotherapy based on CBT principles should be offered. Information about support groups, where they are available, should be offered. (Support groups may provide face-to-face meetings, telephone conference support groups [which can be based on CBT principles], or additional information on all aspects of anxiety disorders plus other sources of help.) The benefits of exercise as part of good general health should be discussed with all patients as appropriate. NICE 2002 – Current research suggests that the delivery of cognitive behavioural therapy via a computer interface (CCBT) may be of value in the management of anxiety and depressive disorders. This evidence is, however, an insufficient basis on which to recommend the general introduction of this technology into the NHS. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 57 Care of people with generalised anxiety disorder Step 1: Recognition and diagnosis of generalised anxiety disorder (as panic disorder, see above) Step 2: Offer treatment in primary care The recommended treatment options have an evidence base: psychological therapy, medication, and self-help have all been shown to be effective. The choice of treatment will be a consequence of the assessment process and shared decision-making. There may be instances when the most effective intervention is not available (for example, cognitive behavioural therapy [CBT]) or is not the treatment option chosen by the patient. In these cases, the healthcare professional will need to consider, after discussion with the patient, whether it is acceptable to offer one of the other recommended treatments. If the preferred treatment option is currently unavailable, the healthcare professional will also have to consider whether it is likely to become available within a useful timeframe. If immediate management of generalised anxiety disorder is necessary, any or all of the following should be considered: • • • • • • Support and information Problem solving Benzodiazepines Sedating antihistamines Self help Benzodiazepines should not usually be used beyond 2 to 4 weeks. In the longer-term care of individuals with generalised anxiety disorder, any of the following types of intervention should be offered and the preference of the person with generalised anxiety disorder should be taken into account. The interventions that have evidence for the longest duration of effect, in descending order are: • Psychological therapy • Pharmacological therapy (antidepressant medication) • Self-help The treatment option of choice should be available promptly. There are positive advantages of services based in primary care (for example, lower rates of people who do not attend) and these services are often preferred by patients. Psychological Interventions CBT should be used. CBT should be delivered only by suitably trained and supervised people who can demonstrate that they adhere closely to empirically grounded treatment protocols. CBT in the optimal range of duration (16-20 hours in total) should be offered. For most people, CBT should take the form of weekly sessions of 1-2 hours and should be completed within a maximum of 4 months of commencement. Briefer CBT should be supplemented with appropriate focussed information and tasks. Where briefer CBT is used, it should be around 8-10 hours and be designed to integrate with structured self-help materials. 58 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Pharmacological Interventions The following must be taken into account when deciding which medication to offer: • • • • • • • • The age of the patient Previous treatment response Risks The likelihood of accidental overdose by the person being treated and by other family members if appropriate The likelihood of deliberate self harm, by overdose or otherwise Tolerability The preference of the person being treated Cost, where equal effectiveness is demonstrated All patients who are prescribed antidepressants should be informed, at the time that treatment is initiated, of potential side effects (including transient increase in anxiety at the start of treatment) and of the risk of discontinuation/withdrawal symptoms if the treatment is stopped abruptly or in some instances if a dose is missed or, occasionally, on reducing the dose of the drug. Patients started on antidepressants should be informed about the delay in onset of effect, the time course of treatment, the need to take medication as prescribed, and possible discontinuation/withdrawal symptoms. Written information appropriate to the patient’s needs should be made available. Unless otherwise indicated, an SSRI should be offered. If one SSRI is not suitable or there is no improvement after a 12-week course, and if a further medication is appropriate, another SSRI should be offered. When prescribing an antidepressant, the healthcare professional should consider the following: Side effects on the initiation of antidepressants may be minimised by starting at a low dose and increasing the dose slowly until a satisfactory therapeutic response is achieved. In some instances, doses at the upper end of the indicated dosage range may be necessary and should be offered if needed. Long-term treatment may be necessary for some people and should be offered if needed. If the patient is showing improvement on treatment with an antidepressant, the drug should be continued for at least 6 months after the optimal dose is reached, after which the dose can be tapered. If there is no improvement after a 12-week course, another SSRI (if another medication is appropriate) or another form of therapy should be offered. Patients should be advised to take their medication as prescribed. This may be particularly important with short half-life medication in order to avoid discontinuation/withdrawal symptoms. Stopping antidepressants abruptly can cause discontinuation/withdrawal symptoms. To minimise the risk of discontinuation/withdrawal symptoms when stopping antidepressants, the dose should be reduced gradually over an extended period of time. All patients prescribed antidepressants should be informed that, although the drugs are not associated with tolerance and craving, discontinuation/withdrawal symptoms may occur on stopping or missing doses or, occasionally, on reducing the dose of the drug. These symptoms are usually mild and self-limiting but occasionally can be severe, particularly if the drug is stopped abruptly. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 59 Healthcare professionals should inform patients that the most commonly experienced discontinuation/withdrawal symptoms are dizziness, numbness and tingling, gastrointestinal disturbances (particularly nausea and vomiting), headache, sweating, anxiety and sleep disturbances. Healthcare professionals should inform patients that they should seek advice from their medical practitioner if they experience significant discontinuation/withdrawal symptoms. If discontinuation/withdrawal symptoms are mild, the practitioner should reassure the patient and monitor symptoms. If severe symptoms are experienced after discontinuing an antidepressant, the practitioner should consider reintroducing it (or prescribing another from the same class that has a longer half-life) and gradually reducing the dose while monitoring symptoms. Self-Help Interventions Bibliotherapy based on CBT principles should be offered. Information about support groups, where they are available, should be offered. (Support groups may provide face-to-face meetings, telephone conference support groups [which can be based on CBT principles], or additional information on all aspects of anxiety disorders plus other sources of help). Large group CBT should be considered. The benefits of exercise as part of good general health should be discussed with all patients as appropriate. NICE 2002 – Current research suggests that the delivery of cognitive behavioural therapy via a computer interface (CCBT) may be of value in the management of anxiety and depressive disorders. This evidence is, however, an insufficient basis on which to recommend the general introduction of this technology into the NHS. Step 3: Review and offer alternative treatment if appropriate If, following a course of treatment, the clinician and patient agree that there has been no improvement with one type of intervention, the patient should be reassessed and consideration given to trying one of the other types of intervention. Step 4: Review and offer referral from primary care if appropriate In most instances, if there have been two interventions provided (any combination of medication, psychological intervention, or bibliotherapy) and the person still has significant symptoms, then referral to specialist mental health services should be offered. If venlafaxine is being considered: Venlafaxine treatment should only be initiated by specialist mental health medical practitioners including General Practitioners with a Special Interest in Mental Health. Venlafaxine treatment should only be managed under the supervision of specialist mental health medical practitioners including General Practitioners with a Special Interest in Mental Health. The dose of venlafaxine should be no higher than 75 mg per day. Before prescribing venlafaxine an initial electrocardiogram (ECG) and blood pressure measurement should be undertaken. There should be regular monitoring of blood pressure and monitoring of cardiac status as clinically appropriate. 60 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Step 5: Care in specialist mental health services Specialist mental health services should conduct a thorough, holistic, re-assessment of the individual, their environment and social circumstances. This reassessment should include evaluation of: • • • • • • • Previous treatments, including effectiveness and concordance Any substance use, including nicotine, alcohol, caffeine, and recreational drugs Comorbidities Day-to-day functioning Social networks Continuing chronic stressors The role of agoraphobic and other avoidant symptoms. A comprehensive risk assessment should be undertaken and an appropriate risk management plan developed. To undertake these evaluations and to develop and share a full formulation, more than one session may be required and should be available. Care and management will be based on the individual’s circumstances and shared decisions arrived at. Options include: • Treatment of comorbid conditions • CBT with an experienced therapist if not offered already, including home based CBT if attendance at clinic is problematic • Structured problem solving • Full exploration of pharmaco-therapy • Day support to relieve carers and family members • Referral for advice, assessment, or management to tertiary centres There should be accurate and effective communication between all healthcare professionals involved in the care of any person with generalised anxiety disorder and particularly between primary care clinicians (GP and teams) and secondary care clinicians (community mental health teams) if there are existing physical health conditions that also require active management. Monitoring and follow up Psychological Interventions There should be a process within each practice to assess the progress of a person undergoing CBT. The nature of that process should be determined on a case-by-case basis. Pharmacological Interventions When a new medication is started, the efficacy and side-effects should be reviewed within 2 weeks of starting treatment and again at 4, 6, and 12 weeks. Follow the Summary of Product Characteristics (SPC) with respect to all other monitoring required. At the end of 12 weeks, an assessment of the effectiveness of the treatment should be made, and a decision made as to whether to continue or consider an alternative intervention. If medication is to be continued beyond 12 weeks, the individual should be reviewed at 8- to 12- week intervals, depending on clinical progress and individual circumstances. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 61 Self-Help Interventions Individuals receiving self-help interventions should be offered contact with primary healthcare professionals, so that progress can be monitored and alternative interventions considered if appropriate. The frequency of such contact should be determined on a case-by-case basis, but is likely to be between every 4 and 8 weeks. Outcome Measures Short, self-complete questionnaires (such as the panic subscale of the agoraphobic mobility inventory for individuals with panic disorder) should be used to monitor outcomes wherever possible. Interventions for Generalised Anxiety Disorder (GAD) Pharmacological compared with psychological compared with combined interventions for GAD If immediate management of GAD is necessary, any or all of the following should be considered: • • • • • • Support and information Problem solving Benzodiazepines Sedative antihistamines Self help Benzodiazepines should not usually be used beyond 2-4 weeks. In the longer-term care of individuals with generalised anxiety disorder, any of the following types of intervention should be offered and the preference of the person with generalised anxiety disorder should be taken into account. The interventions that have evidence for the longest duration of effect, in descending order are: • Psychological therapy • Pharmacological therapy (antidepressant medication) • Self-help The treatment option of choice should be available promptly. There are positive advantages of services based in primary care (for example, lower rates of people who do not attend) and these services are often preferred by patients. Pharmacological interventions for GAD The following must be taken into account when deciding which medication to offer: • The age of the patient • Previous treatment response • Risks • The likelihood of accidental overdose by the person being treated and by other family members if appropriate • The likelihood of deliberate self harm, by overdose or otherwise • Tolerability • The preference of the person being treated • Cost, where equal effectiveness is demonstrated All patients who are prescribed antidepressants should be informed, at the time that treatment is initiated, of potential side effects (including transient increase in anxiety at the start of treatment) and of the risk of discontinuation/withdrawal symptoms if the treatment is stopped abruptly or in some instances if a dose is missed or, occasionally, on reducing the dose of the drug. 62 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Patients started on antidepressants should be informed about the delay in onset of effect, the time course of treatment, the need to take medication as prescribed, and the possible discontinuation/withdrawal symptoms. Written information appropriate to the patient’s needs should be made available. Unless otherwise indicated, an SSRI should be offered. If one SSRI is not suitable or there is no improvement after a 12-week course, and if a further medication is appropriate, another SSRI should be offered. When prescribing an antidepressant, the healthcare professional should consider the following: Side effects on the initiation of antidepressants may be minimised by starting at a low dose and increasing the dose slowly until a satisfactory therapeutic response is achieved. In some instances, doses at the upper end of the indicated dosage range may be necessary and should be offered if needed. Long-term treatment may be necessary for some people and should be offered if needed. If the patient is showing improvement on treatment with an antidepressant, the drug should be continued for at least 6 months after the optimal dose is reached, after which the dose can be tapered. If there is no improvement after a 12-week course, another SSRI (if another medication is appropriate) or another form of therapy should be offered. Patients should be advised to take their medication as prescribed. This may be particularly important with short half-life medication in order to avoid discontinuation/withdrawal symptoms. Stopping antidepressants abruptly can cause discontinuation/withdrawal symptoms. To minimise the risk of discontinuation/withdrawal symptoms when stopping antidepressants, the dose should be reduced gradually over an extended period of time. All patients prescribed antidepressants should be informed that, although the drugs are not associated with tolerance and craving, discontinuation/withdrawal symptoms may occur on stopping or missing doses or, occasionally, on reducing the dose of the drug. These symptoms are usually mild and self-limiting but occasionally can be severe, particularly if the drug is stopped abruptly. Healthcare professionals should inform patients that the most commonly experienced discontinuation/withdrawal symptoms are dizziness, numbness and tingling, gastrointestinal disturbances (particularly nausea and vomiting), headache, sweating, anxiety, and sleep disturbances. Healthcare professionals should inform patients that they should seek advice from their medical practitioner if they experience significant discontinuation/withdrawal symptoms. If discontinuation/withdrawal symptoms are mild, the practitioner should reassure the patient and monitor symptoms. If severe symptoms are experienced after discontinuing an antidepressant, the practitioner should consider reintroducing it (or prescribing another from the same class that has a longer half-life) and gradually reducing the dose while monitoring symptoms. If venlafaxine is being considered: Venlafaxine treatment should only be initiated by specialist mental health medical practitioners including General Practitioners with a Special Interest in Mental Health. Venlafaxine treatment should only be managed under the supervision of specialist mental health medical practitioners including General Practitioners with a Special Interest in Mental Health. The dose of venlafaxine should be no higher than 75 mg per day. Before prescribing venlafaxine an initial ECG and blood pressure measurement should be undertaken. There should be regular monitoring of blood pressure, and monitoring of cardiac status as clinically appropriate. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 63 Psychological interventions for GAD CBT should be used. CBT should be delivered only by suitably trained and supervised people who can demonstrate that they adhere closely to empirically grounded treatment protocols. CBT in the optimal range of duration (16-20 hours in total) should be offered. For most people, CBT should take the form of weekly sessions of 1-2 hours and should be completed within a maximum of 4 months of commencement. Briefer CBT should be supplemented with appropriate focussed information and tasks. Where briefer CBT is used, it should be around 8-10 hours and be designed to integrate with structured self-help materials. Other interventions for GAD Bibliotherapy based on CBT principles should be offered. Information about support groups, where they are available, should be offered. (Support groups may provide face-to-face meetings, telephone conference support groups [which can be based on CBT principles], or additional information on all aspects of anxiety disorders plus other sources of help.) Large group CBT should be considered. The benefits of exercise as part of good general health should be discussed with all patients as appropriate. NICE 2002 – Current research suggests that the delivery of cognitive behavioural therapy via a computer interface (CCBT) may be of value in the management of anxiety and depressive disorders. This evidence is, however, an insufficient basis on which to recommend the general introduction of this technology into the NHS. c) Risk factor/recovery Potential harms • Antidepressants may result in a transient increase in anxiety at the start of treatment. • Selective serotonin reuptake inhibitors (SSRIs) may cause nausea, diarrhoea, headache, dizziness, sexual dysfunction, asthenia, somnolence sweating, changes in blood pressure, and myoclonus. • Potential side effects of buspirone include dizziness, headaches, nausea, nervousness, and paraesthesia. • Stopping antidepressants abruptly can cause discontinuation/withdrawal symptoms. The most commonly experienced discontinuation/withdrawal symptoms are dizziness, numbness and tingling, gastrointestinal disturbances (particularly nausea and vomiting), headache, sweating, anxiety, and sleep disturbances. • Tricyclic antidepressants (TCAs) cause, to varying degrees, anticholinergic side effects (dry mouth, blurred vision, constipation, urinary retention, sweating), sedation, and increase in heart rate. • Serotonin syndrome may develop following co-administration of SSRIs or SSRIs with monoamine oxidase inhibitors (MAOIs) and is potentially life threatening. • Venlafaxine has a broad range of side effects which can increase blood pressure at higher doses and is associated with a high incidence of discontinuation symptoms. • Benzodiazepines side effects include fatigue and insomnia. d) Return to work No stated. 64 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 8. Priority for Q-COMP Rating criteria Functional restoration Does the guideline consider graded increases in activity and function? Psychosocial factors To what degree does the guideline consider psychosocial factors that may influence recovery? Return to work process (vocational rehabilitation) To what degree does the guideline consider the Return to Work Process (vocational rehabilitation)? Risk factors for recovery To what degree does the guideline consider Risk Factors for Recovery? Total rating 3 1 1 2 7 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 65 Guideline for the evaluation and treatment of injured workers with psychiatric conditions Contents 1. 2. 3. 4. 5. 6. 7. Developed by ................................................................................................................................................................................... 44 Guideline status ............................................................................................................................................................................... 44 Where located/how accessed ..................................................................................................................................................... 44 Description/scope .......................................................................................................................................................................... 44 Outcomes considered .................................................................................................................................................................... 46 Agree appraisal................................................................................................................................................................................. 46 Relevance/appropriateness of use in workers’ compensation sector ............................................................................... 46 a) Functional progression ............................................................................................................................................................ 46 b) Physical/psychiatric rehabilitation ........................................................................................................................................ 56 c) Risk factor/recovery ................................................................................................................................................................ 56 d) Return to work........................................................................................................................................................................... 57 8. Priority for Q-COMP ...................................................................................................................................................................... 57 66 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 1. Developed by Washington State Department of Labor and Industries. Guideline for the evaluation and treatment of injured workers with psychiatric conditions. Olympia (WA): Washington State Department of Labor and Industries; 2004.6 p. 2. Guideline status This is the current release of the guideline. This guideline updates a previous version: Washington State Department of Labor and Industries. Guidelines for psychiatric and psychological evaluation of injured or chronically disabled workers. Olympia (WA): Washington State Department of Labor and Industries; 2002 Aug.10 p. 3. Where located/how accessed National Guideline Clearinghouse www.guideline.gov Print copies; L&I Warehouse, Department of Labor and Industries, P.O. Box 44843, Olympia, Washington 98504-4843. 4. Description/scope Disease/condition(s) • Psychiatric conditions suspected of retarding recovery form an industrial injury • Psychiatric conditions caused by an industrial injury • Preexisting psychiatric conditions aggravated by an industrial injury Guideline category • Diagnosis • Evaluation • Management • Treatment Clinical speciality • Psychiatry • Psychology Intended users • Physicians • Psychologists/ Non-physician Behavioural Health Clinicians Guideline objectives To assist psychologists and psychiatrists who treat injured workers for psychiatric conditions that are either the direct result of an industrial injury or are unrelated but retarding recovery from an industrial injury. To assist physicians who treat injured workers’ physical conditions, but who from time to time refer injured workers to psychiatrists or psychologists for treatment of psychiatric conditions. To assist claim managers to validate their decisions, and thus help to ensure efficient medical management of the claim. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 67 Target population Injured workers with diagnosed or suspected psychiatric conditions Interventions and Practices Considered 1. Formulation of a psychiatric diagnosis • Evaluation including review of all relevant historical information • Classification using Diagnostic and Statistical Manual of Mental Disorders, 4th edition (DSM-IV) (or current edition) • Standardized measuring tools, such as Rollins® or Beck® scales, and individualized visual analogue scales. 2. Identification of barriers to recovery from an industrial injury 3. Formulation of a psychiatric treatment plan that addresses each diagnosed psychiatric condition and barriers to recovery • Use of objectively determinable measurements of recovery • Discussion of predictable drug interactions for recommended medications 4. Assessment of psychiatric treatment • Progress notes • Visual analogue scale for assessing a patient’s perception 5. Outcomes considered Not stated. 6. Agree appraisal • • • • • • Scope and Purpose Stakeholder Involvement Rigour of Development Clarity and Presentation Applicability Editorial Independence 61% 36% 24% 36% 0% 25% 7. Relevance/appropriateness of use in workers’ compensation sector a) Functional progression Major recommendations Authorization requirements Initial psychiatric evaluation and ongoing treatment of a psychiatric condition both require prior approval from the department or self-insured employer (WAC 296-21-270). Authorization for psychiatric treatment may be granted for periods of 90 days or less. Subsequent authorization periods of 90 days or less are contingent on documented progress in psychiatric treatment. Claim managers may authorize payment for treatment of psychiatric conditions that are retarding recovery from an industrial injury, even though the injury did not cause the psychiatric condition or aggravate a preexisting psychiatric condition. Claim managers can also authorize payment for treatment of psychiatric conditions when they have been caused or aggravated by an industrial injury. 68 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions If authorization for psychiatric treatment is requested following an initial psychiatric evaluation, it is the claim manager’s responsibility to make a determination as to the relationship between the industrial injury and the psychiatric condition based on the information provided. For this reason, it is very important for the psychiatrist or psychologist to clearly indicate their opinion, and the basis for their opinion, whether: • The injured worker’s psychiatric condition was not caused or aggravated by the industrial injury, but it creates a barrier to recovery from a condition for which the department has accepted liability. • The injured worker’s psychiatric condition was caused by the industrial injury. • The injured worker’s psychiatric condition is a preexisting condition that was aggravated by the industrial injury. • The injured worker’s psychiatric condition was neither caused nor aggravated by the industrial injury, nor is it creating a barrier to recovery from a condition for which the department has accepted liability. Elements of a comprehensive psychiatric plan Elements of a comprehensive psychiatric treatment plan would include formulation of a psychiatric diagnosis; identification of barriers to recovery; development of an intensive, goal-directed plan; and recommendation for duration of therapy. Diagnosis of a psychiatric condition Diagnosis is an essential first step to the development of a plan for treatment of psychiatric conditions. Diagnoses should be specific, and should use the nomenclature and numerical identification of the Diagnostic and Statistical Manual of Mental Disorders, 4th edition (DSM-IV) (or current edition). The diagnostic section of the initial report, and all subsequent reports, should address all five axes described in the DSM-IV (or current edition). Diagnoses should be based on all relevant historical information. Specific inquiry should be made into the patients´ preinjury and current medical, psychosocial, and psychological status. Whenever possible, prior medical records should be reviewed to screen for the presence of diagnostically important information and for information that may be useful in the creation of a treatment plan. Carefully document any pertinent positive or negative historical information. Consideration should be given to the use of standardized measuring tools, such as the Rollins® or Beck® scales, and the use of individualized visual analog scales. Such measurements provide both support for diagnoses and benchmarks against which progress in treatment can be measured. What are the reporting requirements? All reports should be written in a legible style that can be understood by nonmedical personnel. Each report must contain at least a summary of subjective complaints, objective observations, assessment of progress toward meeting goals, updated treatment plan, and DSM-IV (or current edition) axis format assessment (WAC 296-21270). The use of specific examples of a patient’s behavior may be a helpful way to communicate the effects of a psychological condition, or the effects of treatment for such a condition. Doctors treating psychiatric conditions allowed on a claim are required to submit progress reports to the claim manager every sixty days (WAC 296-21-270). If temporary treatment has been authorized for an unrelated psychiatric condition, progress reports are required to be submitted to the claim manager every thirty days (WAC 296-20-055). (Refer to the original guideline document for information on billing codes.) b) Physical/psychiatric rehabilitation Formulation of a psychiatric treatment plan The psychiatrist or psychologist evaluating a worker with a psychiatric condition should create a treatment plan that addresses each diagnosed psychiatric condition and any identified barriers to recovery. The treatment plan Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 69 must include intensive, goal-directed treatment and include a recommended duration of treatment. The treatment plan should be included in the evaluation report and updated throughout treatment. Objectively determinable measurements of recovery should be identified for each condition for which treatment is proposed. Objective measurements should be individualized so that each patient’s progress or lack of progress will be accurately assessed. Examples of such measurements include documentation of the level of physical activity; improved participation in physical therapy, occupational therapy, work hardening, or vocational counseling programs; normalization of common behavior patterns such as sleep cycles and eating disorders; and changes in medication usage. To the extent that a treatment plan may recommend medications, the plan should include a discussion of any predictable drug interactions the recommended medications might have with medications the worker is currently taking. (Refer to the original guideline document for an example of a treatment plan.) Identification of the measured variable should include a description of what will be measured, the intervals and duration during which the variable will be measured, the anticipated endpoint, and the anticipated progress to that endpoint at each interval measurement. When appropriate, use standardized measurements such as the Rollins® or Beck® scales to document the extent of recovery. Each variable to be measured should be explained to the injured worker before treatment is actually commenced. If necessary, the patient should be instructed in how to complete diaries that document such variables as pain, activity, medication use, etc. In the event that the psychiatric treatment plan includes measurements of indicators that are outside the practice of the psychiatrist or psychologist, prior arrangements to obtain such measurements should be made by the psychiatrist or psychologist with the attending doctor. Such measurements should be available to the psychiatrist or psychologist at the time each respective progress note is created. (Refer to the original guideline document for an example of measurements arranged by the psychiatrist or psychologist and the attending doctor.) Assessment of psychiatric treatment and recommendations A progress note should be prepared following each clinic visit. Per WAC 296-20- 06101, legible copies of progress notes must be submitted to the department for all treatment. The progress note should document the patient’s interval history and should summarize any pertinent positive or negative findings. Indicators that are measured to assess progress should be documented along with measurements obtained during the interval period. An assessment should be made as to whether the measurements reflect the expected progress. A visual analog scale can be a useful tool in assessing a patient´s perception. Generally, such scales consist of a 10cm horizontal line with words at opposite ends of the spectrum. Studies have shown that visual analog scales are most accurately representative of that which they seek to measure when the horizontal line contains no arbitrary divisions such as numbers, interval marks, etc. The patient is instructed to place a vertical mark at the point on the line that seems most appropriate to the patient. Should expected progress not be made, the report of the psychiatrist or psychologist should contain a discussion concerning the postulated reasons for lack of progress. If necessary, the treatment plan should be reassessed, and any necessary modifications made. (Refer to the original guideline document for an example of a progress note.) c) Risk factor/recovery Identification of barriers to recovery from an industrial injury Each diagnosed psychiatric condition should be assessed to determine whether it is retarding a patient’s recovery from an industrial injury. Any such barriers should be clearly identified and the report should provide an explanation that links the psychiatric condition to an observable, measurable behavior that interferes with recovery from an industrial injury. (Refer to the original guideline document for an example.) Specific inquiry should be made to determine whether there are employment related risk factors that should be addressed in a health care setting. For example, anger towards the employer, supervisor, or coworkers may need to be addressed. Economic disincentives and employment-related loss of self-esteem can each contribute to the failure of a worker to make expected progress in recovery. Feelings of victimization may delay a return to a normal 70 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions lifestyle. Such risk factors should be carefully identified and documented. d) Return to work Not discussed. 8. Priority for Q-COMP Rating criteria Functional restoration Does the guideline consider graded increases in activity and function? Psychosocial factors To what degree does the guideline consider psychosocial factors that may influence recovery? Return to work process (vocational rehabilitation) To what degree does the guideline consider the Return to Work Process (vocational rehabilitation)? Risk factors for recovery To what degree does the guideline consider Risk Factors for Recovery? Total rating 1 1 2 1 5 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 71 VA/DoD clinical practice guideline for the management of post-traumatic stress Contents 1. 2. 3. 4. 5. 6. 7. Developed by ................................................................................................................................................................................... 73 Guideline status ............................................................................................................................................................................... 73 Where located/how accessed ..................................................................................................................................................... 73 Description/scope .......................................................................................................................................................................... 73 Outcomes considered .................................................................................................................................................................... 77 Agree appraisal................................................................................................................................................................................. 77 Relevance/appropriateness of use in workers’ compensation sector ............................................................................... 77 a) Functional progression ............................................................................................................................................................ 77 b) Physical/psychiatric rehabilitation ......................................................................................................................................104 c) Risk factor/recovery ..............................................................................................................................................................105 d) Return to work.........................................................................................................................................................................107 8. Priority for Q-COMP ....................................................................................................................................................................107 72 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 1. Developed by Veterans Health Administration, Department of Defence. VA/DoD clinical practice guideline for the management of post-traumatic stress. Version 1.0. Washington (DC): Veterans Health Administration, Department of Defense; 2004 Jan. Various p. [479 references] 2. Guideline status This is the current release of the guideline. 3. Where located/how accessed National Guideline Clearinghouse www.clearinghouse.gov Electronic copies; Available in Portable Document Format (PDF) from the Department of Veterans Affairs Web site. Print copies; Available from the Department of Veterans Affairs, Veterans Health Administration, Office if Quality and Performance (10Q) 810 Vermont Ave.NW, Washington, DC 20420 The following companion documents are available: • Various companion documents are available from the: Veterans Health Administration (VHA) Web site. • In addition, the VHA Web site provides references to related guidelines, performance measures, and other resources. • Guideline for guidelines. Draft. Washington (DC): Veterans Health Administration, Department of Veterans Affairs. Available at: VHA Web site. Print copies: Department of Veterans Affairs, Veterans Health Administration, Office of Quality and Performance (10Q) 810 Vermont Ave. NW, Washington, DC 20420. 4. Description/scope Disease/condition(s) • Post traumatic stress disorder Guideline category • Diagnosis • Evaluation • Management • Prevention • Treatment Clinical speciality • Family Practice • Internal Medicine • Psychiatry • Psychology Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 73 Intended users • Health Care Providers • Health Plans • Hospitals • Managed Care Organizations • Nurses • Physician Assistants • Physicians • Psychologists/ Non-physician Behavioural Health Clinicians Guideline objectives To survey best practices in post-traumatic stress disorder prevention, diagnosis, and treatment and to determine whether the evidence supports current practices, or whether the evidence suggests they should be modified or discontinued. Target population Any person who is eligible for care in the Veterans Affairs or Department of Defense health care delivery system, specifically, military men or women and veterans who have survived traumatic events. Interventions and practices considered 1. Initial Evaluation and Triage (includes Primary Prevention) • Education and training to promote hardiness and resiliency • Provide realistic training • Strengthen perceived ability to cope • Create supportive interpersonal work environments • Develop and maintain adaptive beliefs • Develop workplace-specific comprehensive traumatic stress management programs 2. Screen for Post-Traumatic Stress Disorder (PTSD) symptoms • Primary care PTSD Screen • PTSD Brief Screen • Short Screening Scale for Diagnostic and Statistical Manual , 4th editions (DSM IV ) PTSD Management of Acute Stress Reaction (ASR) 1. Screen for ASR 2. Assess medical and functional status based on general appearance and screening instruments 3. Medical status including: • History, physical examination, and a neurological examination • Use of prescribed medications, mood or mind-altering substances, and possible biological or chemical agent exposure • A minimal mental status examination to assess cognitive function • Screen for toxicity • Radiological assessment of patients with focal neurological findings or possible head injury • Appropriate laboratory studies to rule out medical disorders that may cause symptoms of acute stress reactions (e.g., complete blood count [CBC] , chemistry profile, thyroid studies, human chorionic gonadotropin [HCG], electrocardiogram, electroencephalogram) 74 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions • A focused psychosocial assessment • Brief assessment of functioning 4. Ensure basic physical needs are met by protecting, directing, connecting with, and triaging patients. 5. Acute symptom management • Assurance/ reassurance • Defusing (3-phased discussion provided within hours of the crisis for purpose of assessment triage and acute symptom mitigation) • Mitigate fear and anxiety • Sleep hygiene • Re-establish routine • Exercise and nutrition • Bereavement • Survivor success • Advise about alcohol/substance abuse • Modulate mood/irritability 6. Psychological debriefing 7. Facilitate social and Psychological support 8. Pharmacotherapy • Propanolol • Benzodiazepines • Other sympatholytics • Antidepressants • Anticonvulscents • Atypical antipsychotics • Antihistamines • Typical antipsychotics 9. Reassessment after acute intervention by evaluation of risk factors 10. Referral and consultation with mental health professionals Management of Combat and Ongoing Operation Stress Reaction (COSR) 1. Screening for symptoms of COSR 2. Assess risk of harm to self or others 3. Identification of service members who can return to functioning in unit 4. Acute symptom management according to “PIES” principle (proximity, immediacy, expectancy, simplicity) 5. Transfer for treatment, as needed. Management of Acute Stress Disorder (ASD) and Post-Traumatic Stress Disorder (PTSD) in Primary Care 1. Assessment of trauma exposure, trauma-related symptoms, and dangerousness to self or others 2. Obtain medical history, physical examination, mental status examination, laboratory tests, psychological assessment, functional assessment, and other evaluations 3. Patient education 4. Referral to Vet Centers Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 75 Management of Acute Stress Disorder (ASD) and Post-Traumatic Stress Disorder (PTSD) in Specialty Care 1. Mental health assessment 2. Medical history, physical examination, mental status examination, psychosocial assessment, and appropriate lab test 3. Documentation of DSM-IV criteria in medical record 4. Patient and family education 5. Initiation of therapy for PTSD 6. Reassessment of status after therapeutic interventions 7. Follow-up in mental health and referral Evidence-based intervention for treatment of PTSD 1. Cognitive Therapy 2. Exposure Therapy 3. Stress Inoculation Testing 4. Eye Movement Desensitization and Reprocessing 5. Imagery Rehearsal Therapy 6. Psychodynamic Therapy 7. Group Therapy 8. Dialectic Behaviour Therapy 9. Hypnosis 10. Spiritual Support 11. Acute Stress Disorder Pharmacotherapy • Imipramine • Propranolol • Benzodiazepines • Anticonvulscents • Other antidepressants • Other sympatholytics • Atypical antipsychotics • Chloral hydrate • Typical antipsychotics (not recommended) 12. Post-traumatic stress disorder pharmacotherapy using monotherapy and/or augmented therapy for targeted symptoms • Selective serotonin reuptake inhibitors (SSRIs) • Tricyclic antidepressants (TCA’s) • Monoamine oxidase inhibitors (MAOIs) • Sympatholytics • Novel antidepressants • Anticonvulscents • Atypical antipsychotics • Buspirone • Non-benzodiazepines hypnotics • Benzodiazepines (not recommended) • Typical antipsychotics (not recommended) 76 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 5. Outcomes considered • Effect on treatment on Clinician Administered Post-traumatic Stress Disorder Scale (CAPS) or other measures of post-traumatic stress disorder (PTSD) • Effect of treatment on symptoms of PTSD • Relapse rate in persons with PTSD • Prevention of PTSD • Risk factors of PTSD • Sensitivity and specificity of screening tools for PTSD 6. Agree appraisal • • • • • • Scope and Purpose Stakeholder Involvement Rigour of Development Clarity and Presentation Applicability Editorial Independence 67% 46% 60% 92% 11% 17% 7. Relevance/appropriateness of use in workers’ compensation sector a) Functional progression Major recommendations The recommendations for the management of post-traumatic stress are organized into 5 major algorithms. Note: A list of abbreviations is provided at the end of the “Major Recommendations” field. Core module - initial evaluation and triage Primary prevention A. Education and training to promote hardiness and resiliency Objective Prepare individuals and groups for exposure to traumatic experiences in ways that minimize the likelihood of development of post traumatic stress disorder (PTSD) and other trauma-related problems. Recommendations 1. In high-risk occupations for which probability of trauma exposure is moderate or high, efforts should be undertaken to increase psychological resilience of workers to the negative effects of trauma exposure. (Working Group Consensus) B. People at-risk for developing stress symptoms after trauma Objective Identify persons at risk for developing a traumatic stress disorder (PTSD) after trauma exposure. Recommendations 1. Persons exposed to trauma should be assessed for known risk factors for developing PTSD – both pre-trauma risks and post-trauma risks. (Brewin, Andrews, & Valentine, 2000) Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 77 2. The trauma type, nature, and severity should be assessed. (Brewin et al., 1999; Bryant et al., 2000; Harvey & Bryant, 2000; Mellman et al., 2001) 3. Assessment of existing social supports and ongoing stressors is important. (Litz et al., 2002) 4. Patients with Acute Stress Disorder (ASD) warrant careful clinical attention, as they are at high-risk for developing PTSD. (Birmes et al., 2001; Brewin et al., 1999; Bryant et al., 2000, Harvey & Bryant, 2000; Mellman et al., 2001; Murray, Ehlers, & Mayou, 2002) 5. Patients with dissociative symptoms may also warrant careful clinical attention. (Brewin et al., 1999; Murray, Ehlers, & Mayou, 2002 C. Screen for PTSD symptoms Objective Identify possible cases of PTSD. Recommendations 1. All new patients should be screened for symptoms of PTSD (Breslau et al., “Previous exposure,” 1999; Leskin & Westrup, 1999; Prins et al. 1999; Taubman-Ben-Ari et al., 2001) initially and then on an annual basis or more frequently if clinically indicated due to clinical suspicion, recent trauma exposure (e.g., major disaster), or history of PTSD.(Working Group Consensus) 2. Patients should be screened for symptoms of PTSD using paper and pencil or computer-based screening tools. 3. No studies are available that compare the benefits of one PTSD screening tool versus another. However, the following screening tools have been validated and should be considered for use: • Primary Care PTSD Screen (PC-PTSD) • PTSD Brief Screen • Short Screening Scale for DSM IV PTSD (Breslau et al. “Previous exposure,” 1999; Leskin & Westrup, 1999; Prins et al., 1999) 4. There is, as yet, insufficient evidence to recommend special screening or differing PTSD treatment for members of any cultural or racial groups. (Frueh, Brady & de Arellano , 1998; Frueh et al., 1997; Frueh, Smith, & Libet, 1996; Ortega & Rosenheck, 2000; Penk et al., 1989; Rosenheck & Fontana, 1996; Trent et al., 2000) D. Are trauma related symptoms present? Objective Identify people exposed to trauma who are at risk for developing an acute stress reaction (ASR), acute stress disorder (ASD), or post-traumatic stress disorder (PTSD). Recommendations 1. Individuals who are presumed to have symptoms of PTSD or who are positive for PTSD on the initial 4-item screening should receive specific assessment of their symptoms. 2. Useful information may include details such as time of onset, frequency, course, severity, level of distress, functional impairment, and other relevant information. 3. The elapsed time since the exposure to trauma is very important in assessing the risk of developing PTSD and determining the appropriate intervention. See the original guideline document for definitions of stress-related disorders and syndromes that will help providers select the appropriate treatment algorithm. E. Normalization for asymptomatic survivors and responders Objective Help trauma survivors and responders who are NOT themselves experiencing signs or symptoms recognize that these reactions in others are common in the aftermath of trauma and do not signify personal inadequacy, health problems, mental illness, or other enduring negative consequences. 78 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Recommendations 1. Pre- and post-trauma education should include helping asymptomatic trauma survivor or responder understand that the acute stress reactions of other people are common and do not indicate personal failure or weakness, mental illness, or health problems. The responders should be taught the simple words and measures that will support quick recovery, rather than push survivors towards a persisting disorder. (Working Group Consensus); 2. Education should include sufficient review of the many ways that post traumatic problems can present, including symptoms in the ASD/PTSD spectrum, behavioral problems with family and friends, occupational problems, and alcohol or other substance misuse/abuse. 3. Provide education and access information to include the following: • Begin with clear statement about ASR being normal, common, and expectable responses to trauma; the reliance on self and buddy management, and other available resources if stress symptoms persist or worsen. • Maximize positive expectation of mastery. • Demystify PTSD (before listing symptoms) and emphasize the human brain and mind´s natural resiliency (e.g., our forefathers/mothers, generations ago survived very bad situations or we wouldn´t be here, and we can survive also). • Painful memories sometimes get stuck, through no fault of the sufferer. Such memories cause real biological changes that can cause physical change and illness elsewhere in the body. Many of these changes can be reversed. All can be compensated for by developing new brain skills, aided by medication when appropriate. • Professionals with special skills and capabilities (including some religious pastors and mental health professionals, other medical people, and others with special training and supervision) can intervene to reverse this process. • Resolving developing symptoms and problems Module a1 - acute stress reaction (asr) Assessment A. Trauma exposure Definition Traumatic events are events that cause a person to fear that he or she may die or be seriously injured or harmed. These events also can be traumatic when the person witnesses them happening to others. Such events often create feelings of intense fear, helplessness, or horror for those who experience them. Among the common kinds of traumatic events are: • • • • • • • • Combat in a war zone Rape or other sexual assault Natural disaster (e.g., hurricanes, floods, or fires) Child physical and/or sexual abuse Domestic violence (battering) Motor vehicle accidents Exposure to the sudden or unexpected death of others Sudden life-threatening physical illness (e.g., heart attack or cancer) B. Screen for ASR Objective Identify individuals who may be at risk for endangering themselves or others due to emotional distress or functional incapacity. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 79 Recommendations 1. Identification of a patient with ASR symptoms is based on observation of behavior and function. 2. There is no evidence to support any specific screening tool. 3. Individuals exhibiting the following responses to trauma should be screened for ASR: • Physical: exhaustion, hyperarousal, somatic complaints (gastrointestinal [GI], genitourinary [GU], musculoskeletal [MS], cardiovascular [CV], respiratory, nervous system [NS]), conversion disorder symptoms • Emotional: anxiety, depression, guilt/hopelessness • Behavioral: avoidance, problematic substance use • Cognitive/mental: amnestic or dissociative symptoms, hypervigilance, paranoia, intrusive re-experiencing. C. Dangerousness to self or others Objective Protect individuals who may be at risk for endangering themselves or others due to emotional distress or functional incapacity. Recommendations 1. Acute medical issues should be addressed to preserve life and avoid further harm: • ABC´s (Maintain: Airways, Breathing, Circulation) • Substance intoxication or withdrawal • Danger to self or others: suicidal, homicidal behavior • Self-injury or mutilation • Inability to care for oneself 2. A safe private, and comfortable environment should be arranged for continuation of the evaluation. • Establish a working treatment alliance with the patient • Maintain a supportive, nonblaming nonjudgmental stance throughout the evaluation • Help with the removal of any ongoing traumatic event • Minimizing further traumas that may arise from the initial traumatic event • Assess and optimize social supports 3. Legal mandates should be followed: • Reporting of violence, assault • Confidentiality for the patient • Mandatory testing • Attend to chain of evidence in criminal cases (e.g., rape, evaluation) • Involuntary Commitment procedures if needed 4. Carefully consider the following potential interventions to secure safety: • Find safe accommodation and protecting against further trauma • Voluntary Admission • Restraint/seclusion only if less restrictive measures are ineffective • Forced medications 80 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions D. Assess medical and functional status based on general appearance and screening instruments Recommendations 1. Medical status should be obtained for all persons presenting with symptoms to include: • History, physical examination, and a neurological examination • Use of prescribed medications, mood or mind-altering substances, and possible biological or chemical agent exposure • A minimal mental status examination to assess cognitive function 2. The history and physical examination findings should lead the provider to other assessments as clinically indicated. There is no test for acute stress reaction, so testing is directed towards detection of associated medical conditions. Assessment may include: • Screen for toxicology if the symptom presentation indicates • Radiological assessment of patients with focal neurological findings or possible head injury • Appropriate laboratory studies to rule out medical disorders that may cause symptoms of acute stress reactions (e.g., complete blood count [CBC], chemistry profile, thyroid studies, human choriogonadotropin [HCG}, electrocardiogram [EKG], electroencephalography [EEG]) 3. A focused psychosocial assessment should be performed including active stressors, losses, current social supports, basic needs (e.g. housing, food, financial resources). 4. A brief assessment of function based on general appearance and behavior should be completed to evaluate: 1) objectively impaired function; 2) subjectively impaired function; 3) baseline level of function (LOF) vs. current LOF; and 4) family and relationship functioning. The approach to triage in the immediate response to traumatic exposure for service members with symptoms during Ongoing Military Operations may vary markedly from the management of civilians exposed to traumatic events. Combat and Operational Stress Reactions (COSR) management is targeted to preserve the fighting force and return the service member (SM) to functional status. See module A2 - Management of Combat and Operational Stress Reaction (COSR) E. Assess preexisting psychiatric and medical conditions Recommendations 1. Assessment of patients with preexisting psychiatric conditions to identify the vulnerable, high-risk individuals and groups 2. Referral to mental health specialty when indicated or emergency hospitalization if needed. F. Risk factors for developing ASD/PTSD Recommendations 1. Individuals exposed to trauma should be screened for one or more of the following risk factors for developing ASD/PTSD. Pre-traumatic factors: • • • • Ongoing life stress Lack of social support Preexisting psychiatric disorder Other pre-traumatic factors including: female gender, low socioeconomic status, lower level of education, lower level of intelligence, race (Hispanic, Japanese, other ethnic minority), reported abuse in childhood, report of other previous traumatization, report of other adverse childhood factors, family history of psychiatric disorders, poor training or preparation for the traumatic event • Peri-traumatic or trauma related factors: • Severe trauma Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 81 • • • • • Type of trauma (interpersonal traumas such as torture, rape, or assault convey high risk of PTSD) High perceived threat to life Age at trauma (school age youth, 40–60 years of age) Community (mass) trauma Other peri-traumatic factors including: history of peri-traumatic dissociation and interpersonal trauma Post-traumatic factors: • • • • • Ongoing life stress Lack of social support Bereavement Major loss of resources Other post-traumatic factors including children at home and female with distressed spouse Triage and treatment G. Ensure basic physical needs are met Objective Ensure trauma-exposed persons with acute stress symptoms have their basic needs met. Recommendations 1. Acute intervention should ensure that the following needs are met: Basic Needs: • • • • • • • Safety/security/survival Food, hydration, clothing, and shelter Sleep Medication (i.e., replace medications destroyed/lost) Orientation Communication with family, friends, and community Protection from ongoing threats/toxins/harm Psychological First Aid: • • • • • • 82 Protect survivors from further harm Reduce physiological arousal Mobilize support for those who are most distressed Keep families together and facilitate reunion with loved ones Provide information, foster communication and education Use effective risk communication techniques Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions H. Acute symptom management Recommendations 1. Symptoms treatment should be provided after basic needs are met (e.g., sleep, normalization, and other nonpharmacological modalities). 2. Apply a series of specific psychological interventions (individually or in a group) to reduce acute stress symptoms and to address both general recovery and specific symptoms (e.g., breathing/relaxation treatment). Individual psychological interventions may include: • Assurance/reassurance • Defusing (3-phased discussion provided within hours of the crisis for purpose of assessment triage and acute symptom mitigation) • Mitigate fear and anxiety • Sleep hygiene • Reestablish routine • Exercise and nutrition • Bereavement • Survivor success • Advise about alcohol/substance use • Modulate mood/irritability Group psychological interventions: • Groups may be effective vehicles for providing trauma-related education, training in coping skills, and increasing social support especially in the context of multiple group sessions. • Group participation should be voluntary. 3. Peoples´ reaction to ASR varies. Some want and feel a need to discuss the event, and some have no such need. Respect individual and cultural preferences in the attempt to meet their needs as much as possible. Allow normal recovery, and monitor. 4. Consider a short course of medication for some individuals targeted for specific symptoms (e.g., sleep disturbance). [See Annotation M ] I. Psychological debriefing Objective Reduce risk for development of PTSD following traumatic event. Recommendation Individual: 1. 1. Recommend against psychological debriefing as a viable means of reducing acute post-traumatic distress (ASR or ASD) or progression to PTSD. (Hobbs et al., 1996; Mayou, Ehlers, & Hobbs, 2000; Bisson et al., 1997 Group: 2. 1. There is insufficient evidence to recommend for or against conducting structured group debriefing. 3. 2. Compulsory repetition of traumatic experiences in a group may be counterproductive. 4. 3. Group debriefing with preexisting groups (teams, units, Emergency Medical Teams [EMTs], co-workers, family members) may assist with group cohesion, morale, and other important variables that have not been demonstrated empirically. (Foa, Keane, & Friedman, 2000; Rose, Bisson, & Wessely, 2002) 5. 4. Group participation should be voluntary. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 83 J. Education and normalization / expectancy of recovery Recommendation 1. All survivors should be given educational information to help normalize common reactions to trauma, improve coping, enhance self-care, facilitate recognition of significant problems, and increase knowledge of and access to services. Such information can be delivered in many ways, including public media, community education activities, and written materials. K. Facilitate social and spiritual support Recommendation 1. Preserve an interpersonal safety zone protecting basic personal space (e.g., privacy, quiet, personal effects). 2. Provide nonintrusive ordinary social contact (e.g., a “sounding board,” judicious use of humor, small talk about current events, silent companionship). 3. Provide opportunities for grieving for losses. Provide access to religious/spiritual resources when sought. (Providing space and opportunities for prayers, mantras, rites and rituals, and end-of-life care as determined important by the patient) 3. Consider providing direct spiritual care or ensuring patient access to spiritual care when sought. Evidence 1. Consider referral for religious/spiritual counseling as indicated for patient symptoms, consistent with available resources, and resonant with patient belief systems (Baldacchino & Draper, 2001; Bell Meisenhelder, 2002; Calhoun et al., 2000; Humphreys et al., 2001; Nixon et al., 1999; Strawbridge et al., 1998) 2. When providing psychological first aid or primary care services, consider providing direct spiritual care or ensuring patient access to spiritual care (Bogia & Preston, 1985; Everly, “The role of pastoral crisis,” 2000) 3. For patients who have developed PTSD, consider referral for religious/spiritual counseling as indicated for patient symptoms, consistent with available resources, and resonant with patient belief systems (Baldacchino & Draper, 2001; Bell Meisenhelder, 2002; Calhoun et al., 2000; Humphreys et al., 2001; Nixon et al., 1999; Strawbridge et al., 1998) Objective To lessen the physical, psychological, and behavioral morbidity associated with acute stress reaction, hasten the return to full function (duty), and diminish the likelihood of chronicity Recommendations Summary Table – Pharmacotherapy for ASR R* Significant Benefit Some Benefit Unknown No Benefit/Harm A B C I Propanolol Benzodiazapines Other aympatholytics Antidepressants Anticonvulscents Atypical antipsychotics Antihistamines D *R = Level of recommendation 84 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Typical antipsychotics 1. Strongly recommend providing for physical needs, sleep, normalization, and other non-pharmacological modalities. 2. Recommend the use of medication only for individuals that do not respond to non-pharmacological treatment as a normal recovery is expected from ASR. 3. Consider a short course of medication targeted for specific symptoms. • Sleep disturbance/insomnia (e.g., benzodiazepines, antihistamines) • Hyperarousal/excessive arousal/panic attacks. (e.g., benzodiazepines, propranolol [up to 10 days]) 4. There is insufficient evidence to support a recommendation for preventative use of a pharmacological agent to prevent the development of ASD or PTSD. Evidence 1. Benzodiazepines (Mellman, Byers, & Augenstein, 1998) 2. Antihistamines 3. Propranolol (Pitman et al., 2002) 4. Pharmacotherapy prophylaxis for ASD or PTSD (Stein et al., 2000) M. Reassessment Objective Identify patients with persistent traumatic stress symptoms, related dysfunction, or additional treatment needs. Recommendations 1. Treatment response to the acute intervention should be reassessed. This should include an evaluation for the following risk factors: • Persistent or worsening traumatic stress symptoms (e.g., dissociation, panic, autonomic arousal, cognitive impairment) • Significant functional impairments (e.g. role/work, relationships) • Dangerousness (suicidal or violent ideation, plan, and/or intent) • Severe psychiatric comorbidity (e.g., psychotic spectrum disorder, substance use disorder or abuse) • Maladaptive coping strategies (e.g., pattern of impulsivity, social withdrawal under stress) • New or evolving psychosocial stressors • Poor social supports 2. Follow-up after acute intervention to determine patient status. • Patient does not improve or status worsens – refer to mental health provider and/or PTSD specialty team. Recommend continued involvement of the primary care provider in the treatment. Patients with multiple problems may benefit from a multi-disciplinary approach to include occupational therapy, spiritual counseling, recreation therapy, social work, psychology, and/or psychiatry. • Patient demonstrates partial improvement (e.g., less arousal, but no improvement in sleep) – consider augmentation or adjustment of the acute intervention within 2 weeks. • Patient recovers from acute symptoms – provide education about acute stress reaction and contact information with instructions for available follow-up if needed. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 85 Follow-up N. Referral and consultation with mental health Objective Provide guidance for primary care providers on optimal referral for potential PTSD patients. Recommendations 1. Individuals who exhibit any of the following conditions should be referred to mental health: • Failure to respond to acute supportive interventions • Worsening of stress related symptoms • High potential for dangerousness • Development of ASD/PTSD • New onset of dangerousness or maladaptive coping to stress • Exacerbation of pre existing psychiatric conditions • Deterioration in function • New onset stressors, poor social supports, or inadequate coping skills. O. Monitor and follow-up Recommendations 1. Follow-up should be offered to those individuals who request it. 2. Follow-up should be offered to individuals and groups at high risk of developing adjustment difficulties following exposure to major incidents and disasters, including individuals who: • Have ASD or other clinically significant symptoms stemming from the trauma • Are bereaved • Have a preexisting psychiatric disorder • Have required medical or surgical attention • Were exposed to a major incident or disaster that was particularly intense and of long duration Module a2 – combat and ongoing operation stress reaction (cosr) The approach to triage in the immediate response to traumatic exposure for service members with symptoms during Ongoing Military Operations is directed by dual sets of objectives: Military considerations Management of combat and operational stress reactions (COSR) during ongoing military operations is targeted to preserve the fighting force and return the service member (SM) to functional status. Context and setting of care delivery may vary markedly. Military clinical objectives 1. Prevent exacerbation of symptoms/mitigate symptoms of acute stress 2. Prevent development of traumatic stress sequelae (e.g., ASD, PTSD, depressive disorders, anxiety disorders, and substance use disorders) 3. Keep SM with his/her unit and prevent unnecessary medical evacuation 4. Return SM to duty as soon as possible 5. Maintain and enhance unit capabilities and readiness Prior to deployment and regularly thereafter, ensure appropriate primary prevention in the form of COSR briefs are offered to combatants, providers, and the chain of command. NOTE: For further discussion of the key element, please see Module A1: Acute Stress Reaction. 86 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions A. Service member with symptoms Of Combat And Operational Stress Reaction (COSR) During ongoing military operations Recommendations 1. Identify service member with symptoms compatible with COSR. Symptoms are not attributed to identified medical/surgical condition requiring other urgent treatment (a service member can have COSR concurrent with minor return-to-duty [RTD] wounds/illness) 2. Evacuate to next level of care, if unmanageable 3. Screen service member for symptoms of COSR, which include: • Exhaustion/burnout • Hyperarousal and anxiety • Somatic complaints (gastrointestinal, genitourinary, musculoskeletal, cardiovascular, respiratory, nervous system) • Depression or guilt/hopelessness • Conversion Disorder symptoms • Amnestic or dissociative symptoms • Behavioral changes • Emotional dysregulation • Anger/irritability • Brief, manageable “psychotic symptoms” (e.g., hallucination due to sleep deprivation and mild “paranoia”) 4. Address the underlying cause of symptoms (e.g., sleep deprivation) in brief restoration program. Advise service member´s Commander, chaplain, etc. on follow-up actions. Document symptoms and observations. B. Assess risk of harm to self or others; seek collateral information about stressors, and service member´s function, medical history, and absence or impairment on operation or mission Objective Obtain information to assess service member´s condition and triage for appropriate care. Recommendations 1. Arrange for a safe and comfortable environment to continue the evaluation. Secure any weapons and explosives. 2. Medical triage to rule out: • Neurotoxicant exposure • Head injury • Undetected wounds • Acute physical illness (e.g., infectious) 3. Document symptoms of COSR, obtain collateral information from unit leaders, and assess service member´s function, to include: • Any changes in productivity? • Coworker or supervisor reports of recent changes in appearance, quality of work, or relationships? • Any tardiness/unreliability, loss of motivation, or loss of interest? • Forgetful or easily distracted? • Screening for substance use Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 87 C. Can service member return to duty within hours? Objective Identify service members who can rapidly resume effective functioning in the unit. Recommendations 1. Consider the service member’s role and functional capabilities and the complexity and importance of his/her job when determining when to return the service member to duty. 2. The continuing presence of symptoms of COSR alone should not constitute a basis for preventing a return to duty. 3. Educate and “normalize” observed psychological reactions to the chain of command. D. Initiate acute intervention for COSR; Coordinate with service member´s unit/command; treat within closest proximity to service member´s unit, as is logistically feasible Objective Initiate acute symptom management. Recommendations 1. Maintain sense of unit integrity: • Normalization • Validation • Keep positive approach • Set up expectation for recovery and RTD (role) 2. Keep treatment consistent with the “PIES” principle: • Proximity: Prevention and treatment are conducted in proximity to the battlefield or the origin of the stressor. Treatment proximate to the member´s unit where he/she can be visited by fellow military members is ideal. Consider all options for proximate treatment; strive to maintain connection to unit to maintain unit integrity • Immediacy: Treatment should begin as soon as tactically and logistically possible • Expectancy: From the outset, the expectation is that the SM is experiencing a normal reaction to an abhorrently abnormal situation and will return to duty following resolution, restitution and adaptation • Simplicity: All modalities of prevention and treatment are simple and clearly understood. No dynamic therapy. No medical model. The only “model” is the military model—military members caring for military members. 3. Initiate treatment: • Treat according to SM´s prior role and not as a “patient;” avoid a hospital setting • Assure or provide the following, as needed: • Reunion or contact with primary group • Respite from intense stress • Thermal comfort • Oral hydration • Oral food • Hygiene (toileting, shower, shave, and feminine) • Sleep (to facilitate rest and restoration, use anxiolytic medication judiciously and sparingly in the acute setting) • Encourage talk about the event with supportive others 4. Reserve group debriefing for members of preexisting and continuing groups at appropriate time and setting. Attendance should be voluntary and only be conducted by personnel trained in debriefing methods 5. Assign job tasks and recreational activities that will restore focus and confidence and reinforce teamwork (limited duty) 6. Avoid further traumatic events until recovered for full duty 88 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 7. Evaluate periodically 8. Consider using a short course of medication targeted for specific symptoms (see “Pharmacotherapy for COSR” in the original guideline document) E. Transfer to more definitive level of care for combat and operational stress control Objective Transfer service member for treatment augmentation or mental health treatment or referral. Recommendations 1. Service members who do not respond to first line supportive interventions may warrant a transfer for treatment augmentation or mental health treatment or referral. 2. Transfer to a more definitive level of treatment may include more intense or prolonged treatment at a Combat Refresher Training facility. Service members should be prepared for the transfer with continued positive expectation of recovery from their symptoms and return to normal level of functioning. 3. Ensure that casualties being transferred due to other medical conditions (wounded in action) receive psychoeducation relating to anticipated psychological changes, provide positive expectations, and offer support prior to departure from the area of responsibility. Module B: acute stress disorder (asd) and post-traumatic stress disorder (ptsd) in primary care A. Assessment of trauma exposure related symptoms Recommendations Assessment in Primary Care 1. Patients who are presumed to have symptoms of PTSD or who are positive for PTSD on the initial screening should receive specific assessment of their symptoms. (For a list of “Common Symptoms After Exposure to Trauma or Loss,” see Table B-1 in the original guideline document.) 2. A thorough assessment of the symptoms is necessary for accurate diagnosis, rating the severity of the disorder, and making correct clinical decisions. (Lagomasino, Daly, & Stoudemire , 1999; Williams & Shepherd, 2000); 3. Consider self-administered checklists to ensure systematic, standardized, and efficient review of the patient´s symptoms. 4. Useful information may include details such as time of onset, frequency, course, severity, level of distress, functional impairment, and other relevant information. B. Assessment of trauma exposure Recommendations 1. Assessment of the trauma exposure should include: • History of exposure to traumatic event(s) • Nature of the trauma • Severity of the trauma • Duration and frequency of the trauma • Age at the time of the trauma • Patient´s reaction at time of trauma (e.g., helplessness, horror, and fear) • Existence of multiple traumas 2. When assessing trauma exposure, the clinician must consider the patient´s ability to tolerate the recounting of traumatic material, since it may exacerbate PTSD symptoms. 3. The assessment should be performed cautiously, especially in situations where the trauma source is still present and the patient perceives himself or herself to be in danger. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 89 C. Assessment of dangerousness to self or others Recommendation 1. All patients with ASD/PTSD should be assessed for safety and dangerousness including current risk to self or others, as well as historical patterns of risk: • Suicidal or homicidal ideation, intent (plan), means (e.g., weapon, excess medications), history (e.g., violence or suicide attempts), behaviors (e.g., aggression, impulsivity), comorbidities (substance abuse, medical conditions) (Breslau at al., 2000; Bullman & Kang, 1994; Ferrada-Noli et al., 1998; Kaslow et al., 2000; Marshall et al., 2001; Prigerson & Slimack, • 1999; Swanson et al., 2002 • Family and social environment – including risks to the family (Seng, 2002; Swanson et al., 2002) • Ongoing health risks or risk-taking behavior (Acierno et al., 1996; Hutton et al., 2001) • Medical/psychiatric comorbidities or unstable medical conditions (Davidson et al., 1991; Farrell & Ganzini, 1995; Weisberg et al., 2002) • Consider potential to jeopardize mission in operational environment (Working Group Consensus) D. Obtain medical history, physical examination, mental status examination (MSE), and laboratory tests Objective Obtain comprehensive patient data in order to reach a working diagnosis. Recommendations 1. All patients should have a thorough medical and psychiatric history (Lagomasino, Daly, & Stoudemire, 1999; Williams & Shepherd, 2000), with particular attention paid to the following: • Baseline functional/mental status • Past medical history • Medications, to include herbal and over-the-counter (OTC) drugs • Past psychiatric history, to include prior treatment, past hospitalization for depression or suicidality, and substance use disorders • Current life stressors If trauma exposure is recent (<1 month) particular attention should be given to the following: • • • • Exposure to/environment of trauma Ongoing traumatic event Exposure, perhaps ongoing, to environmental toxin Ongoing perceived threat 2. All patients should have a thorough physical examination. On physical examination, particular attention should be paid to the neurological exam and stigmata of physical/sexual abuse, self-mutilation, or medical illness. Note distress caused by or avoidance of diagnostic tests/examination procedures. 3. All patients, particularly the elderly, should have a Mental Status Examination (MSE) to include assessment of the following: • Appearance and behavior • Language/speech • Thought process (loose associations, ruminations, obsessions) and content (delusions, illusions, and hallucinations) • Mood (subjective) • Affect (to include intensity, range, and appropriateness to situation and ideation) 90 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions • Level of Consciousness (LOC) • Cognitive function 4. All patients should have routine laboratory screening tests including thyroid stimulating hormone (TSH), Complete Metabolic Panel, Hepatitis, human immunodeficiency virus (HIV), and human choriogonadotropin (HCG) (for females). Also consider CBC, urinalysis (UA), toxicology ethanol (Tox EtoH) panel and other tests, as clinically indicated. (Lagomasino, Daly & Stoudemire, 1999; Williams & Shepherd, 2000) 5. Other assessments may be considered (radiology studies, EKG, and EEG), as clinically indicated. (Lagomasino, Daly & Stoudemire, 1999) 6. All patients should have a narrative summary of psychological assessments to include work/school, family, relationships, housing, legal, financial, unit/community involvement, and recreation, as clinically appropriate. E. Assessment of functioning Recommendation 1. Assessment of global function should be obtained, such as the Global Assessment of Function (GAF) scale or the SF-36. (Working Group Consensus) F. Assessment of risk factors (See under Risk Factors/Recovery below) G. Are there clinical significant symptoms suggestive of PTSD or ASD? Recommendations 1. Primary care providers should formulate a presumptive diagnosis of stress related disorder consistent with Diagnostic and Statistical Manual of Mental Disorders (4th edition) criteria for ASD and PTSD. 2. Primary care providers should consider initiating treatment or referral based on a working diagnosis of stress related disorder. 3. Patients with difficult or complicated presentation of the psychiatric component should be referred to mental health specialty for diagnosis and treatment. Evidence for all Recommendations: H. Patient education Objective Help trauma survivors cope with ASD/PTSD by providing information that may help them manage their symptoms and benefit from treatment. Recommendation 1. Trauma survivors should be educated about PTSD symptoms, other potential consequences of exposure to traumatic stress, practical ways of coping with traumatic stress symptoms, processes of recovery from ASD/ PTSD, and the nature of treatment. (Working Group Consensus) I. Coexisting severe medical conditions Objective Improve management of PTSD symptoms when they are complicated by the presence of a medical or psychiatric comorbidity. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 91 Recommendations 1. Primary care providers should recognize that medical disorders/symptoms, mental disorders, and psychosocial problems commonly coexist with PTSD and should screen for them during the evaluation and treatment of PTSD. (Working Group Consensus) 2. Consider the existence of comorbid conditions when deciding whether to treat patients in the primary care setting or refer them for specialty mental health care. (Working Group Consensus) J. Concurrent PTSD and substance abuse Objective Improve the management of PTSD symptoms when they are complicated by a concurrent substance abuse problem. Recommendations 1. Substance use patterns of clients with trauma histories or PTSD should be routinely assessed (see the VA/DoD Clinical Practice Guideline for the Management of Substance Use Disorders) (Working Group Consensus) 2. Substance abusers should be routinely screened for trauma exposure and PTSD. (Dansky et al., 1997) 3. Integrated PTSD-Substance Abuse Treatment should be considered. (Working Group Consensus) 4. Substance-abusing patients with PTSD should be educated about the relationships between PTSD and substance abuse, referred for concurrent PTSD treatment, or provided with integrated PTSD/Substance Abuse treatment. (Working Group Consensus; Najavits, 2002; Ouimette et al., 1998) 5. Substance Abuse-PTSD patients should receive follow-up care that includes a continued focus on PTSD issues. (Ouimette et al., 2000) K. Referral to mental health specialty Objective Provide guidance for primary care providers on optimal referral for PTSD patients. Recommendations 1. Primary care providers should consult with a mental health provider and/or a PTSD Specialty Team for all patients with acute or chronic stress disorders. 2. Primary care providers should continue to be involved in the treatment of patients with acute or chronic stress disorders. 3. Treatment for patients with ASD or acute or chronic PTSD should involve a multidisciplinary team approach to include occupational therapy (OT), spiritual counseling, recreation therapy, social work, psychology, and/or psychiatry. 4. Patients with clinically significant symptoms or comorbidities to PTSD, including chronic pain, insomnia, anxiety, and depression, should receive treatment for those complicating problems. 5. Case management should be provided, as indicated, to address high utilization of medical resources. 6. Consider referral for alternative care modalities as indicated for patient symptoms, consistent with available resources, and resonant with patient belief systems. Evidence for all recommendations: L. Treatment in primary care Recommendations ALL PATIENTS with Stress Related Disorders 1. A supportive and collaborative treatment relationship or therapeutic alliance should be developed and maintained with patients with ASD/PTSD inclusive of their input in treatment planning. 92 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 2. Primary care providers should routinely provide the following services for all patients with stress related disorders, especially those who are reluctant to seek specialty mental health care: • Supportive counseling • PTSD-related education • Regular follow-up and monitoring of symptoms • Early recognition of PTSD 3. Primary care providers should consider consultation with mental health providers for patients with ASD/PTSD who warrant a mental health referral but may be reluctant or refuse it. 4. Primary care providers should take leadership in convening a collaborative team for patients with PTSD. Team members may include the primary care providers, mental health specialists, chaplains, pastors, social worker, occupational or recreational therapists, Vet Centers, family support centers, exceptional family member programs, VA benefit counselors, peer-support groups, and others. ASD 5. Because ASD does not occur in all people who later develop PTSD, consider treatment for acutely traumatized people with ASD, with severe PTSD symptoms as well as for those who are incapacitated by acute psychological or physical symptoms. 6. Patients with ASD should be monitored for development of PTSD (Brewin et al., 1999; Bryant et al., 1998). The use of validated PTSD symptom measure such as the PTSD Checklist should be considered (see Appendix D in the original guideline document). 7. Primary care providers should consider the pharmacological management of disruptive symptoms (e.g., sleep) (see “Pharmacotherapy for ASD” in the original guideline document). 8. Brief intervention (4 to 5 sessions) of cognitive behavioral therapy (CBT) is an effective early intervention for patients with ASD (Bryant et al., 1998; Foa et al., 1995). In addition to targeted brief interventions, some trauma survivors may benefit from follow-up provision of ongoing counseling or treatment. PTSD 9. All patients with PTSD should have a specific primary care provider assigned to coordinate their overall health care. 10. Pharmacological management of PTSD or related symptoms may be initiated based on a presumptive diagnosis of PTSD. Long-term pharmacotherapy will be coordinated with other intervention once the patient has been referred to a mental health clinic (see “Pharmacotherapy for PTSD” in the original guideline document). 11. Primary care providers should perform a brief PTSD symptom assessment at each visit. The use of a validated PTSD symptom measure, such as PTSD Checklist, should be considered (see Appendix D in the original guideline document). 12. Primary care providers should assess patients with PTSD for associated high-risk behaviors (e.g., smoking, alcohol/drug abuse, HIV, and hepatitis risks) and comorbid medical and psychiatric illnesses. M. Referral to vet centers Objective Provide timely mental health services to veterans in need of support. Recommendations 1. Veterans with symptoms of PTSD should have an initial assessment of needs. 2. Veterans who are dangerous to self or others should be referred to the local Veterans Affairs Medical Center (VAMC) or nearest emergency room. 3. Veterans who are seeking to have basic needs met should be referred to the VA Homeless Coordinator or community resources for food, shelter, or emergency financial assistance. 4. Veterans who are eligible for Vet Center services should have an indepth psychological history taken, including a comprehensive military history and treatment plan. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 93 5. Treatment plans in the Vet Center may include individual, family, or group therapy. Veterans can receive medical treatment or medication management at the Vet Center by a psychiatrist, registered nurse (RN), or advanced registered nurse practitioner (ARNP) or be referred to the local VAMC, Community Based Outpatient Clinic (CBOC), or community resources. 6. Veterans who are eligible for Vet Center services should be made aware of the Center resources and referred if the patient desires. N. Assess duty/work responsibilities and patient´s fitness (in relation to military operation) Recommendations 1. The determination of when to return a service member to duty should take into consideration the individual´s service member´s role, the complexity and importance of his or her job, and the service member´s functional capabilities. 2. The continuing presence of symptoms of PTSD should not be considered as the sole basis for preventing a return to duty. Module c management of ptsd in mental health speciality care A. Patient presenting to mental health with suspected PTSD symptoms Recommendations Assessment in Mental Health Specialty 1. Mental health clinicians should obtain a comprehensive diagnostic assessment that includes, but is not limited to, the symptoms that characterize PTSD. 2. Routine use of self-administered checklists may ensure systematic, standardized, and efficient review of the patient´s symptoms and history of trauma exposure (see Appendix C [PCL-C] in the original guideline document). 3. The assessment should also include review of other salient symptoms (guilt, dissociation, derealization, depersonalization, reduction, and awareness of surrounding) that impact on treatment decisions. Structured psychiatric interviews, such as the clinician administered PTSD scale (CAPS), may be considered. For discussion see CORE Module Annotation D, and Module B – Management of ASD and PTSD in Primary Care Annotations A and B B. Obtain medical history, physical examination, mse, psychosocial assessment, and appropriate lab tests See Module B: Management of ASD & PTSD in Primary Care, Annotation D, E and F. C. Does Patient Meet DSM-IV Criteria For ASD/PTSD? Objective Diagnose ASD/PTSD by DSM-IV criteria. Recommendation 1. Diagnostic criteria should be documented in the medical record. D. Educate patients and family about treatment options; develop collaborative and interdisciplinary treatment plan See Module B: Management of ASD & PTSD in Primary Care, Annotation H. 94 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions E. Initiate Therapy for PTSD See Intervention Module. F. PTSD with other Comorbid Symptoms (Addiction, Substance Use Disorder [SUD], Psychosis, Bipolar) See Module B: Management of ASD & PTSD in Primary Care, Annotation I & J. G. Reassess PTSD Symptoms; diagnostic status, functional status; quality of life; additional treatment needs; patient preferences Objective Assess patient status following therapeutic intervention to determine future direction. Recommendations 1. Follow-up status of patients with PTSD should be monitored at least every three months. Use interview and questionnaire methods to assess PTSD symptoms and function. • Diagnostic status and symptom severity • Functional status/health-related quality of life • Psychosocial treatment needs • Patient preferences • Therapy adherence • Adverse treatment effects H. Follow-up in mental health Recommendations 1. If patient does not improve or status worsens, consider one of the following treatment modification options: • Continued applications of the same modality at intensified dose and/or frequency • Change to a different treatment modality • Apply adjunctive therapies • Increase level of care (e.g., referral facility, partial hospitalization, inpatient hospitalization, residential care) • Consider a referral to adjunctive services for treatment for comorbid disorders or behavioral abnormalities (e.g., homelessness, domestic violence, or aggressive behavior) 2. If patient demonstrates partial (insufficient) remission, consider one of the following treatment modification options: • Continue the present treatment modality to allow sufficient time for a full response • Continue applications of the same modality at intensified dose and/or frequency • Change to a different treatment modality • Apply adjunctive therapies • Increase level of care (e.g., referral facility, partial hospitalization, inpatient hospitalization, residential care) • Consider a referral to adjunctive services for treatment of comorbid disorders or behavioral abnormalities (e.g., homelessness or domestic violence) 3. If patient demonstrates improved symptoms and functioning but requires maintenance treatment: • Continue current course of treatment • Consider stepping down the type, frequency, or dose of therapy Transition from intensive psychotherapy to case management contacts • Transition from individual to group treatment modalities • Discuss patient status and need for monitoring with the primary care provider • Consider a referral to adjunctive services for treatment of disorders or behavioral abnormalities (e.g., Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 95 • • • • homelessness or domestic violence) If patient demonstrates remission from symptoms and there are no indications for further therapy: Discontinue treatment Educate the patient about indication and route of future care access Monitor by primary care for relapse/exacerbation. I. Referral Objective Treat symptoms, support function, and alleviate suffering in those patients with PSTD who are unwilling, unable, or unsuitable for treatment in a mental health setting. Recommendations 1. Evaluate psychosocial function and refer for psychosocial services, as indicated. Available resources include, but are not limited to chaplains, pastors, Family Support Centers, Exceptional Family Member Programs, VA benefit counselors, occupational or recreational therapists, Vet Centers, and peer-support groups. 2. Provide case management, as indicated, to address high utilization of medical resources. 3. Consider psychotherapeutic interventions as appropriate for level of training and available resources. 4. For patients with severe symptoms or coexisting psychiatric problems consider referrals to: • • • • Specialized PTSD programs Specialized programs for coexisting problems and conditions Partial psychiatric hospitalization or “day treatment” programs Inpatient psychiatric hospitalization Evidence for all Recommendations: (Working Group Consensus) Evidence-based intervention for treatment of PTSD Acute Stress Disorder (ASD) Pharmacotherapy Summary table – Pharmacotherapy for ASD R* Significant Benefit Some Benefit Unknown No Benefit/Harm A B C I Imipramine Propanolol Benzodiazepines Other Sympatholitics Other Antidepressants Anticonvulscents Atypical Antipsychotics Chloral Hydrate D Typical Antipsychotics Although the effectiveness of selective serotonin reuptake inhibitors (SSRIs) has been demonstrated for PTSD, it has not been tested in ASD and therefore cannot be recommended. Objective 96 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions To lessen the physical, psychological, and behavioral morbidity associated with acute stress reaction, hasten the return to full function (duty, work, social function), and diminish the likelihood of chronicity. Recommendations 1. Recommend providing for physical needs, sleep, normalization, and other non-pharmacological modalities (Working Group Consensus 2. Consider the use of medication for individuals that do not respond to non-pharmacological treatment (Working Group Consensus) 3. Consider the use of imipramine to ameliorate the symptoms of ASD 4. Consider a short course of medication targeted for specific symptoms Sleep disturbance/insomnia • • • • • Benzodiazepines (up to 5 days) (Gelpin et al., 1996; Mellman, Byers, & Augenstein, 1998) Chloral hydrate (up to 5 days) (Robert et al., 1999) Hyperarousal/excessive arousal/panic attacks Propranolol and other anti-adrenergic agents (up to 10 days) (Pittman et al., 2002) Imipramine (up to 7 days) (Robert et al., 1999) • Benzodiazepines (up to 5 days) avoid short acting agent (e.g., alprazolam) (Gelpin et al., 1996; Mellman, Byers, & Augenstein, 1998) 5. There is insufficient evidence to support a recommendation for preventative use of a pharmacological agent to prevent the development of PTSD. 6. There is insufficient evidence to support a recommendation for PTSD pharmacotherapies for patient presenting symptoms for less than 4 weeks. B. Post-Traumatic Stress Disorder (PSTD) Pharmacotherapy Summary Table for PTSD Pharmacotherapy* R* Significant Benefit A B SSRI’s Some Benefit Unknown No Benefit/Harm C I D TCAs MAOs Sympatholitics Novel Antidepressants Anticonvulscents Atypical Antipsychotics Buspirone Nonbenzodiazepine Hypnotics Benzodiazepines Typical Antipsychotics *R = level of recommendation; SSRIs = selective serotonin reuptake inhibitors; TCAs = tricyclic antidepressants; MAOIs = monoamine oxidase inhibitors. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 97 Objective To minimize signs and symptoms of PTSD and maintain function. Recommendations Monotherapy 1. Strongly recommend selective serotonin reuptake inhibitors (SSRIs) for the treatment of PTSD. (Stein et al., 2000) 2. Recommend tricyclic antidepressants (TCAs) and monoamine oxidase inhibitors (MAOIs) as second-line treatments for PTSD. (Stein et al., 2000; Cochrane Review) 3. Consider an antidepressant therapeutic trial of at least 12 weeks before changing therapeutic regimen. (Martenyi et al., 2002) 4. Consider a second-generation (e.g., nefazodone, trazodone, venlafaxine, mirtazapine, bupropion) in the management of PTSD. (Hidalgo et al., 1999) Augmented Therapy for Targeted Conditions 5. Consider prazosin to augment the management of nightmares and other symptoms of PTSD. (Raskind et al., 2003) 6. Recommend medication compliance assessment at each visit. (Group Consensus) 7. Since PTSD is a chronic disorder, responders to pharmacotherapy may need to continue medication indefinitely; however, it is recommended that maintenance treatment should be periodically reassessed. (Rapaport, Endicott, & Clary, 2002) 8. There is insufficient evidence to recommend a mood stabilizer (e.g., lamotrigine) for the treatment of PTSD. (Hertzberg et al., 1999) 9. There is insufficient evidence to recommend atypical antipsychotics for the treatment of PTSD. (Hamner et al., 2003) 10. There is insufficient evidence to support the recommendation for a pharmacological agent to prevent the development of PTSD. 11. Recommend against the long-term use of benzodiazepines to manage core symptoms in PTSD. (Kosten et al., 2000) 12. Recommend against typical antipsychotics in the management of PTSD. (Stein et al., 2000) 98 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions C. Psychotherapy interventions Objective Reduce symptoms severity and improve of global functioning. Summary Table for Psychotherapy Interventions R* Significant Benefit A Cognitive Therapy (CT) Exposure Therapy (ET) Stress Inoculation Training (SIT) Eye Movement Desensitization And Reprocesssing (EMDR) Some Benefit Unknown No Benefit/Harm B Imagery Rehearsal Therapy (IRT) Psychodynamic Therpy Sympatholitics Novel Antidepressants C I D PTSD-Patient Education *R = level of recommendation Recommendations 1. Providers should explain to all patients with PTSD the range of available and effective therapeutic options for PTSD. (Expert Consensus) 2. Cognitive Therapy (CT), Exposure Therapy (ET), Stress Inoculation Training (SIT), and Eye Movement Desensitization and Reprocessing (EMDR) are strongly recommended for treatment of PTSD in military and non-military populations. EMDR has been found to be as effective as other treatments in some studies and less effective than other treatments in some other studies. 3. Imagery Rehearsal Therapy [IRT] and Psychodynamic Therapy may be considered for treatment of PTSD. 4. Patient education is recommended as an element of treatment of PTSD for all patients. 5. Consider Dialectical Behavioral Therapy (DBT) for patients with a borderline personality disorder typified by parasuicidal behaviors. 6. Consider hypnotic techniques especially for symptoms associated with PTSD, such as pain, anxiety, dissociation and nightmares, for which hypnosis has been successfully used. 7. Specialized PTSD psychotherapies may be augmented by additional problem specific methods/services and pharmacotherapy. 8. Combination of cognitive therapy approaches (e.g., ET plus CT), while effective, has not proven to be superior to either component alone. Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 99 9. Specific psychotherapy techniques may not be uniformly effective across all patients. When selecting a specific treatment modality, consideration of patient characteristics such as gender, type of trauma (e.g., combat vs. other trauma), and past history may be warranted. 10. Patient and provider preferences should drive the selection of evidence-based psychotherapy and/or evidencebased pharmacotherapy as the first line treatment. 11. Selection of individual interventions should be based upon patient preference, provider level of skill and comfort with a given modality, efforts to maximize benefit and minimize risks to the patient, and consideration of feasibility and available resources. 12. Psychotherapies should be provided by practitioners who have been trained in the particular method of treatment, whenever possible. 13. A stepped care approach to therapy administration may be considered, though supportive evidence is lacking. *Detailed evidence tables for each therapy are included in the applicable following Discussion sections. Note: Psychotherapy interventions are aimed at reduction of symptoms severity and improvement of global functioning. However, the clinical relevance and importance of other outcome indicators (e.g., improvement of quality of life, physical and mental health) are not currently well known. A. Selection of therapy for PTSD In clinical practice, providers and patients alike are often faced with important decisions relating to type, number, frequency, and dose of various psychotherapies and pharmacologic therapies. Therapies may be broadly divided into (1) evidence-based psychotherapies, (2) evidence-based pharmacotherapies, and (3) key adjunctive or supplemental treatment modalities. Providers should explain to all patients with PTSD the range of therapeutic options that are available and effective for PTSD. This discussion should include general advantages and disadvantages (including side-effects) associated with each therapeutic option. In general, PTSD therapy research has provided insufficient evidence to favor medication or evidence-based psychotherapy as a first-line treatment. There is also insufficient evidence to suggest for or against combined medication and psychotherapy over only one of the two approaches. It may be helpful to add therapies using a stepped care approach, even though supporting evidence does not exist. The use of stepped care has been advocated for many chronic conditions including hypertension, low back pain, and depression. In stepped care, the intensity of care is augmented for patients who do not achieve an acceptable outcome with lower levels of care. Stepped care is based on three assumptions: different people require different levels of care; finding the right level of care often depends on monitoring outcomes; and moving from lower to higher levels of care based on patient outcomes often offers efficient increases in overall effectiveness. The level or intensity of care is guided by illness trajectory (degree of chronicity and current illness severity), observed outcomes, and previously attempted therapies. Active follow-up is used to determine the level of care each patient requires over time. In PTSD for example, the patient and provider may determine that the first-line therapy will be psychotherapy. If, after a period of treatment, the patient is not responding adequately, the patient may be “stepped up” in therapeutic intensity by adding a medication, such as a selective serotonin reuptake inhibitor (SSRI) to the regimen of ongoing psychotherapy. Contrary to clinical intuition, there is no evidence indicating the superiority of programs that combine different cognitive behavioral therapies. B. Cognitive Therapy (CT) Recommendations 1. CT is effective with civilian men and women exposed to combat and noncombat trauma. (Lovell, et al., 2001; Marks et al., 1998) 2. CT is effective with military and veterans with combat- and noncombat-related PTSD. (Working Group Consensus) 3. CT is effective for women with PTSD associated with sexual assault. (Resick et al., 2002) 100 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions C. Exposure therapy Recommendations 1. ET is effective in the treatment of PTSD (compared to placebo or waiting list) (Cooper & Clum, 1989; Foa et al., 1991; Foa et al., “A comparison,” 1999; Ironson et al., 2002; Keane et al., 1989; Marks et al., 1998; Tarrier et al., 1999) 2 ET compared to other forms of therapy show equivalent results (Foa et al., 1991; Foa et al., “A comparison,”1999; Marks et al., 1998; Paunovic & Ost, 2001; Resnick & Nishisth, 2001; Schnurr, 2001; Tarrier et al., 1999) D. Stress Inoculation Training (SIT) Recommendations 1. SIT is effective as a treatment for PTSD related to sexual assault (Foa et al., 1991; Foa et al., “A comparison,” 1999; Kilpatrick, Veronen, & Resick, 1982; Rothbaum et al., 2000) E. Eye Movement Desensitization and Reprocessing (EMDR) Recommendations 1. EMDR is more efficacious for PTSD than wait-list, routine care, and active treatment controls. (Chemtob, Tolin, & van der Kolk, 2000; Davidson & Parker, 2001; Foa & Meadows, 1997; Maxfield & Hyer, 2002; Shepherd, Stein, & Milne, 2000) 2. Eye movements are not critical to the effects of EMDR (Foa & Meadows, 1997) 3. EMDR compared with ET and CT shows mixed results (Cahill, 2000; Davidson & Parker, 2001; Foa & Meadows, 1997; Ironson et al., 2002; Lee et al., 2002; Power et al., 2002; Servan-Schrieber, 2000; Shepherd, Stein, & Milne, 2000; Taylor, Thordarson, & Maxfield, 2002; Van Etten & Taylor, 1998) F. Imagery Rehearsal Therapy (IRT) Recommendations 1. IRT can be considered for treatment of PTSD (nightmare and sleep disruption in particular). (Krakow et al., 1995; Krakow et al., “Imagery rehearsal,” 2001; Krakow et al., “Treatment of chronic nightmares,” 2001; Forbes, Phelps, & McHugh, 2001) G. Psychodynamic therapy Recommendations 1. Psychodynamic psychotherapy for the treatment of PTSD (Brom, Kleber, & Defares, 1989) 2. Psychodynamic psychotherapy for patients with complex PTSD (Courtois, 1999; Roth & Batson, 1997; Shengold, 1989) H Patient education Objective Provide a therapeutic intervention that reduces the symptoms and functional impairments of PTSD. Recommendation 1. Psychoeducation is recommended (Foa, Davidson, & Frances, 1999) Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 101 I. Group therapy Objective Provide a supportive environment in which a patient with PTSD may participate in therapy with other PTSD patients. Recommendations 1. Consider group treatment for patients with PTSD (Donovan, Padin- Rivera, & Kowaliw, 2001; Foy et al., 2000; Rogers et al., 1999) 2. Current findings do not favor any particular type of group therapy over other types. (Foy et al., 2000) J. Dialectical behavior therapy 1. Consider DBT for patients with a borderline personality disorder typified by parasuicidal behaviors. (Evans et al., 1999; Hawton et al., 2000; Linehan, Heard, & Armstrong, 1993; Safer, Telch, & Agras, 2001; Telch, Agras, & Linehan, 2001; van den Bosch et al., 2002; Verheul et al., 2003) K. Hypnosis Objective A therapeutic intervention that may be an effective adjunctive procedure in the treatment of PTSD Recommendation 1. Hypnosis may be used to alleviate PTSD symptoms. (Brom, Kleber, & Defares, 1989; Sherman, 1998) L. Psychosocial adjunctive methods/services Objective Provide a therapeutic intervention that facilitates generalizing skills for coping with PTSD from clinic to home/ work/community. Recommendations 1. Consider psychosocial rehabilitation techniques once the client and clinician identify the following kind of problems associated with the diagnosis of PTSD: persistent high-risk behaviors, lack of self care/independent living skills, homelessness, interactions with a family that does not understand PTSD, socially inactive, unemployed, and encounters with barriers to various forms of treatment/rehabilitation services. 2. Client and clinician should determine whether such problems are associated with core symptoms of PTSD and, if so, then ensure that rehabilitation techniques are used as a contextual vehicle for alleviating PTSD symptoms. 3. Psychosocial rehabilitation should occur concurrently or shortly after a course of treatment for PTSD, since psychosocial rehabilitation is not trauma-focus. M. Spiritual support Objective Reduce symptoms of PTSD and improve patient´s functioning through social and spiritual support. Recommendation 1. Provide access to religious/spiritual resources, if sought. Evidence Provide opportunities to vent & defuse, to share feelings and talk (Bogia & Preston, 1985; Everly, “The role of pastoral crisis,” 2000; Hunter, 1996) 102 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions Abbreviation/Acronym List ABCs Airway, breathing, circulation AHCPR Agency for Healthcare Policy and Research APA American Psychiatric Association ASD Acute stress disorder ASR Acute stress reaction AUDIT Alcohol Use Disorders Identification Test CAGE Alcohol abuse/dependence screening test mnemonic CAPS Clinician Administered PTSD Scale CBC Complete blood count CBT Cognitive Behavioral Therapy CCTR Cochrane Central Register of Controlled Trials CDR Commander CNS Central nervous system COSR Combat and operational stress reactions CISD Critical Incident Stress Debriefing CT (Interventions) Cognitive Therapy CT Computed tomography CV Cardiovascular DARE Database of Abstracts of Reviews of Effectiveness DAST Drug Abuse/Dependence Screener DBT Dialectical Behavioral Therapy DoD Department of Defense DSM-IV Diagnostic and Statistical Manual of Mental Disorders (4th edition) DTE Direct Therapeutic Exposure EBM Evidence-based medicine EBPTU Evaluation and Brief PTSD Treatment Unit EEG Electroencephalography EKG Electrocardiogram EMDR Eye Movement Desensitization and Reprocessing EMTs Emergency Medical Teams ESRT Emotional Self-Regulation Therapy EtoH Ethanol ET Exposure Therapy FDA U. S. Food and Drug Administration GAF Global Assessment of Function GI Gastrointestinal GU Genitourinary HCG Human Choriogonadotropin HIV Human immunodeficiency virus IRT Image Rehearsal Therapy LOC Level of consciousness LOF Level of function MAOIs Monoamine oxidase inhibitors Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 103 MAST Michigan Alcohol Screening Test MDD Major Depressive Disorder MHP Mental health providers MI Myocardial infarction MMSE Mini-Mental State Examination MRI Magnetic resonance imaging MSE Mental status examination NIMH National Institute of Mental Health NS Nervous system OMO Ongoing military operations OTC Over-the-counter PCL-C PTSD Checklist – Civilian Version PCL-M PTSD Checklist – Military Version PCL-S PTSD Checklist – Stressor Specific Version PCP Primary care provider PE Physical examination PE (Interventions) Prolonged Exposure PIES Proximity, Immediacy, Expectancy, Simplicity PTSD Post-traumatic Stress Disorder QE Quality of evidence RCS Readjustment Counseling Services RCT Randomized controlled trial RTD Return-to-duty SC Supportive Counseling SIADH Syndrome of inappropriate antidiuretic hormone SIPU Specialized Inpatient PTSD Unit SIT Stress Inoculation Therapy SM Service member SR Strength of recommendation SSRI Selective Serotonin Reuptake Inhibitors SUD Substance Use Disorder SUNY State University of New York TCAs Tricyclic Antidepressants TSH Thyroid Stimulating Hormone USPSTF U.S. Preventive Service Task Force VA Veterans Affairs VAMC Veterans Affairs Medical Center VHA Veterans Health Administration b) Physical/psychiatric rehabilitation Discussed extensively throughout “Functional Progression” c) Risk factor/recovery 104 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions F. Assessment of risk factors Recommendations 1. All patients should be assessed for risk factors for developing ASD or PSTD. Special attention should be given to post-traumatic factors (i.e., social support and functional incapacity) that may be modified by intervention. 2. Because of the high prevalence of psychiatric comorbidities in the PTSD population, assessment for depression and other psychiatric comorbidities is warranted (see also VA/DoD Clinical Practice Guideline for the Management of MDD and Psychotic Disorders). 3. Substance use patterns of persons with trauma histories or PTSD should be routinely assessed to identify substance misuse or dependency (alcohol, nicotine, prescribed drugs, and illicit drugs) (see also VA/DoD Clinical Practice Guideline for the Management of Substance Use Disorders) Evidence Pre-trauma 1. Prior exposure to traumatic events (Breslau et al., “Previous exposure” 1999; Brewin, Andrews, & Valentine, 2000; Dougall et al., 2000; Green et al., 2000; Maes et al., 2001; Neria, Bromet, & Marshall, 2002; Ozer et al., 2003; Seedat & Stein, 2000; Zatzick et al., 2002) 2. Female gender (Breslau, “Gender differences,” 2002; Breslau et al., “Vulnerability,” 1999; Brewin, Andrews, & Valentine, 2000, I; Finnsdottir & Elklit, 2002; Neria, Bromet, & Marshall, 2002; Seedat & Stein, 2000; Stretch, Knudson, & Durand, 1998; Zatzick et al., 2002) 3. Psychiatric disorders or personality dimensions (Breslau, “Epidemiologic studies,” 2002; Brewin, Andrews, & Valentine, 2000; Maes et al., 2001; Norris et al., 2002; Ozer et al., 2003) 4. Cognitive factors: Lower intelligence, Neurological soft signs (Brewin, Andrews, & Valentine, 2000; Gurvits et al., 2000) 5. Parental or family history of PTSD (Yehuda et al., 1998) 6. Childhood abuse/assault (Breslau et al., “Previous exposure,” 1999; Breslau, “Epidemiologic studies,” 2002; Brewin, Andrews, & Valentine, 2000; Neria, Bromet, & Marshall, 2002 7. Low educational level or socioeconomic status (Armenian et al., 2000; Brewin, Andrews, & Valentine, 2000; Bromet et al., 2002; Finnsdottir & Elklit, 2002) Peri-trauma 8. Severity of trauma; Perceived life threat (Armenian et al., 2000, II; Brewin, Andrews, & Valentine, 2000; Feehan et al., 2001; Ozer et al., 2003; Woods, 2000) 9. Peri-traumatic dissociation (Ozer et al., 2003) 10. Youth at time of exposure (Brewin, Andrews, & Valentine, 2000; Finnsdottir & Elklit, 2002; Neria, Bromet, & Marshall, 2002; Norris et al., 2002) 11. Biological factors such as heart rate (HR) increase (Shalev et al., “A prospective study,” 1998; Yehuda, McFarlane, & Shalev, 1998) Post-trauma 12. Resource loss/unemployment (Feehan et al., 2001; Norris et al., 2002) 13. Impaired social support system (Armenian et al., 2000; Brewin, Andrews, & Valentine, 2000; Gregurek et al., 2001; Ozer et al., 2003) 14. Health problems (Norris et al., 2002) 15. On-going life stress (Brewin, Andrews, & Valentine, 2000; Norris et al., 2002) Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 105 Potential harms A detailed recounting of a traumatic experience may cause further distress to the patient and is not advisable unless a provider has been trained and is able to support the patient through this experience. Pharmacological adverse effects Note: See Table 4 of Module 1 – Treatment Interventions for PTSD – for detailed list of drug adverse effects and cautions. • Selective serotonin reuptake inhibitors (SSRIs) (fluoxetine, paroxetine, sertraline, fluvoxamine, citalopram): nausea, headache, sexual dysfunction, hyponatremia/syndrome of inappropriate antidiuretic hormone (SIADH), serotonin syndrome • Tricyclic antidepressants (imipramine, amitriptyline, desipramine, nortriptyline, protriptyline, clomipramine): anticholinergic effects, orthostatic hypotension, increased heart rate, ventricular arrhythmias • Monoamine oxidase inhibitors (phenelzine, tranylcypromine): hypertensive crisis with drug/tyramine interactions, bradycardia, orthostatic hypotension, insomnia • Sympatholytics: propranolol – hypotension, bronchospasm, bradycardia; prazosin – first dose syncope • Novel antidepressants: trazodone and nefazodone – sedation, rare priapism; venlafaxine – hypertension in patients with preexisting hypertension;nefazodone – hepatoxicity • Anticonvulsants: carbamazepine – leukopenia, SIADH, drowsiness, ataxia; gabapentin – sedation, ataxia; lamotrigine - Stevens-Johnson syndrome, fatigue; topiramate – secondary angle closure glaucoma, sedation, dizziness, ataxia; valproate – nausea/vomiting, sedation, ataxia, thrombocytopenia • Benzodiazepines (clonazepam, lorazepam, alprazolam, diazepam): sedation, memory impairment, ataxia, dependence • Typical antipsychotics (chlorpromazine, haloperidol, thioridazine): sedation, orthostatic hypotension (with chlorpromazine and thorazine), akathisia, dystonia, drug-induced parkinsonism, tardive dyskinesia , neuroleptic malignant syndrome, QTc changes • Atypical antipsychotics (olanzapine, quetiapine, risperidone): sedation, weight gain, neuroleptic malignant syndrome, akathisia (at high doses), druginduced parkinsonism, especially with doses >6 mg/d • Non-benzodiazepine hypnotics (zaleplon, zolpidem): sedation, ataxia, rebound insomnia • Non-benzodiazepine anti-anxiety (buspirone): nausea, headache Contraindications • Selective serotonin reuptake inhibitors (SSRIs) (fluoxetine, paroxetine, sertraline, fluvoxamie, citalopram) are contraindicated with MAO inhibitor use within 14 days and relatively contraindicated in patients with hypersensitivity. • Tricyclic Antidepressants (imipramine, amitriptyline, desipramine, nortriptyline, protriptyline, clomipramine) are contraindicated with monoamine oxidase inhibitor (MAOI) use within 14 days, and acute myocardial infarction within 3 months, and relatively contraindicated in patients with coronary artery disease and prostatic enlargement. Clomipramine is contraindicated in patients with seizure disorder. • Monoamine Oxidase Inhibitors (MAOI)(phenelzine, tranylcypromine) are contraindicated with use of all antidepressants within 7 days of start of MAOI, except fluoxetine is 5 weeks, and use of central nervous system stimulants and decongestants. • Propranolol: Sinus bradycardia, congestive heart failure are contraindications. • Novel antidepressants (bupropion, nefazodone, trazodone, venlafaxine) are contraindicated with MAOI use within 14 days, and bupropion. • Anticonvulsants: Carbamazepine is contraindicated in patients with bone marrow suppression, particularly leukopenia. Gabapentin is contraindicated in those with renal impairment. Lamotrigine is contraindicated in patients who experience increased rash with valproate (max. dose of 200 mg). Topiramate is contraindicated in patients with hepatic impairment, and valproate with impaired liver function and thrombocytopenia. 106 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions • Benzodiazepines (clonazepam, lorazepam, alprazolam, diazepam) should be used with caution in elderly patients and patients with impaired liver function, and there is a risk of abuse in patients with history of substance abuse. • Typical antipsychotics (chlorpromazine, haloperidol, thioridazine) are contraindicated in patients with Parkinson´s disease and QTc prolongation. • Atypical antipsychotics (olanzapine, quetiapine, risperidone) are relatively contraindicated in Parkinson´s disease. • Non-benzodiazepine hypnotics (zaleplon, zolpidem) should be used with caution with alcohol/drug abuse history and with caution in elderly patients with liver dysfunction. • Non-benzodiazepine anti-anxiety (buspirone) is contraindicated with MAOI use within 14 days. • Contraindications for Cognitive Therapy have not been empirically established, but may include psychosis, severe brain damage, or severe intellectual impairment. • Patients living in dangerous circumstances (e.g., domestic violence or a threatening environment) are not candidates for Exposure Therapy until their security can be assured. Other contraindications for Exposure Therapy have not been confirmed in empirical research, but may include health problems that preclude exposure to intense physiological arousal, current suicidal ideation, substance abuse not in stable remission, comorbid psychosis, or lack of motivation to undergo the treatment. • Contraindications for Group Therapy include active psychosis, severe organicity or limited cognitive capacity, pending litigation, or compensation seeking. • There are a number of contraindications for using traditional hypnotic techniques in the treatment of PTSD: • In the rare cases of individuals who are refractory or minimally responsive to suggestions, hypnotic techniques may not be the best choice, because there is some evidence that hypnotizability is related to treatment outcome efficacy. • Some PTSD patients may be reluctant to undergo hypnosis, either because of religious belief or other reasons. If the resistance is not cleared after dispelling mistaken assumptions, other suggestive techniques can be tried, including emotional self-regulation therapy (ESRT), which is done with open eyes and uses sensory recall exercises rather than a hypnotic induction. • For patients who have low blood pressure or are prone to fall asleep, hypnotic procedures such as “alert hand,” which emphasize alertness and activity rather than relaxation, may be substituted. • Psychosocial rehabilitation techniques are contraindicated when client and clinician conclude that the problems are resolved. • Marriage counseling is typically contraindicated in cases of domestic violence, until the batterer has been successfully (individually) rehabilitated. d) Return to work See above Can Service Member Return To Duty Within Hours. 8. Priority for Q-COMP Rating criteria Functional restoration Does the guideline consider graded increases in activity and function? Psychosocial factors To what degree does the guideline consider psychosocial factors that may influence recovery? Return to work process (vocational rehabilitation) To what degree does the guideline consider the Return to Work Process (vocational rehabilitation)? Risk factors for recovery To what degree does the guideline consider Risk Factors for Recovery? Total rating 4 3 2 1 10 Clinical Guidelines for the Queensland Workers’ Compensation Scheme Psychiatric Conditions 107