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Chronic Pain: New understanding paradigm approach Professor Milton Cohen St Vincent’s Campus, Sydney, and Faculty of Pain Medicine, ANZCA 9 May 2016 To be covered: Comprehensive assessment of patients with CNCP Managing the social and psychological dimensions Pharmacological management Opioid prescription: when and how Other biomedical interventions Philosophies and types of PMPs Facilitating self management “Johnny, are you in pain?” “No, Mummy. The pain is in me.” The Advertiser, 1927 Quoted in The Lancet , 30 June 2012 “Your pain is the breaking of the shell that encloses your understanding.” Kahlil Gibran “To have pain is to have certainty; to hear about pain is to have doubt.” Elaine Scarry, 1985 Courtesy of Prof Deborah Schofield Themes Complex biology of pain Sociopsychobiomedicala ssessment and management Not a “broken part” but a changed person “The body” is not the only thing Therapy of pain, including opioids Self-management is the aim PAI N An unpleasant sensory and emotional experience associated with actual or potential tissue damage or described in terms of such damage PAI N An unpleasant sensory and emotional experience associated with actual or potential tissue damage or described in terms of such damage A dominant paradigm… Biomedical focus Anatomical determinism Dualism …shift Biopsychosocial Sociopsychobiomedical Neural plasticity Interactionism Biomedical Model PAIN (nervous system) DISEASE Problems with Biomedical Model of Pain Implies hard-wired certainty Absence of nociception defaults to “psychogenesis” Excludes narrative of the sufferer CNCP is a complex phenotype [Campbell et al, Pain 2015;156:231-242; NDARC, UNSW Australia] N=1514, CNCP taking prescribed opioids for >6 weeks Low rates of employment/ income Multiple “pain conditions”, poor physical health ~30% abuse/neglect ~ 50% depression; ~25% anxiety; >40% suicidal ideation >30% concurrent BZD; >50% concurrent antidepressant 1:8 cannabis use disorder; 1:3 alcohol use disorder Anterior cingulate cortical (ACC) activation Thermal injury Rectal distention Hearing pain words Viewing facial expressions of pain Social exclusion A model regarding brain circuitry involved in the transition from acute to chronic pain. Apkarian et al. Pain 2011:152:S49-S64 Socio psycho social psycho Bio biomedical ENVIRONMENT PERSON BRAIN AND NERVOUS SYSTEM BODY ENVIRONMENT PERSON BRAIN AND NERVOUS SYSTEM BODY What’s happening in your world (“socio-) What’s happening to you as a person (-”psycho-”) What’s happening to your body (-biomedical”) DISTRESS BELIEFS CULTURE DISABILITY MEMORY EDUCATION NOCICEPTION BLACK FLAGS BLUE FLAGS ORANGE FLAGS YELLOW FLAGS RED FLAGS Early detection of problems? •Symptoms persisting past “healing” •New pathology •Iatrogenic factors ORANGE FLAGS •Unhelpful beliefs about injury •Poor coping strategies •Passive role in recovery BLUE FLAGS •Threats to financial security •Sense of injustice •Litigation RED FLAGS •Mental health disorders •Personality disorders YELLOW FLAGS •Low social support •Unpleasant work •Low job satisfaction •Excessive work demands •Problems outside of work BLACK FLAGS RED FLAGS •Symptoms persisting past “healing” •New pathology •Iatrogenic factors Tenderness - Allodynia Pain in response to a non-noxious mechanical stimulus pressure, movement) Increased responsiveness threshold) of nociceptors (touch, (lower UNDERSTANDING “TENDERNESS” Complaint of pain Hyperalgesia/allodynia Hyperalgesia/allodynia in area of disease, damage or inflammation (1°) in clinically normal tissue (2°) Peripheral sensitisation Central sensitisation CENTRAL SENSITISATION OF NOCICEPTION “Switch-on” of nociceptive pathways in the central nervous system (spinal cord and brain) “Pain…might not necessarily reflect the presence of a peripheral noxious stimulus.” “Pain could…become the equivalent of an illusory perception…” Woolf C. Pain 2011;152:S2-S15 NOCICEPTIVE BARRAGE UNDAMPENED STRESS RESPONSE NERVE DAMAGE SENSITISATION OF CENTRAL NOCICEPTIVE PATHWAYS SPONTANEOUS PAIN ALLODYNIA SPREAD OF PAIN CLINICAL FEATURES SUGGESTING CENTRAL SENSITISATION Absence of obvious tissue damage or disease Sensitivity to touch, movement Worsening pain after repetitive use (hyperpathia) DIAGNOSTIC IMPLICATIONS OF CENTRAL SENSITISATION “Top-down” AND “bottom-up” Avoid chasing nociception in region of pain No language (yet) A FALSE DICHOTOMY “NOCICEPTIVE” “NEUROPATHIC” REPLACING THE DICHOTOMY See Kosek E et al. Do we need a third mechanistic descriptor for chronic pain states? Pain 2016, in press “NOCICEPTIVE” “NOCIPLASTI C” “NEUROPATHIC” THERAPEUTIC IMPLICATIONS OF CENTRAL SENSITISATION Avoid chasing nociception in region of pain Nervous system re-education Pharmacological modification of symptoms and excitability A dominant paradigm shift Biomedical focus Anatomical determinism Dualism Sociopsychobiomedical Neural plasticity Interactionism Our point of view as observers does not allow us to know what it is like to be the system being observed Adolphs & Damasio 1995 Risks – to the patient - of having chronic pain Challenge observers’ view of the world Reinforce clinicians’ uncertainty Fail to validate health professionals’ effectiveness Marginalisation Discrimination Stigmatisation Risks – to the clinician – of chronic pain View of the world challenged Uncertainty reinforced Effectiveness not validated “Negempathy” Conscious avoidance of compassion Negative projection CLINICAL ENCOUNTER SOCIAL DETERMINANTS L A N G U A G E CLINICAL ENCOUNTER ILLNESS BEHAVIOUR EMPATHY HONESTY PSYCHOLOGICAL DISTRESS ATTITUDES & BELIEFS EXPERIENCE TOLERANCE PREJUDICE HOSTILITY SUSPICION CLINICAL BEHAVIOUR AFFECT ATTITUDES & BELIEFS KNOWLEDGE REFRAMING THE ENCOUNTER Shared expertise Neurobiology Empathy Language To be covered: Comprehensive assessment of patients with CNCP Managing the social and psychological dimensions Pharmacological management Opioid prescription: when and how Other biomedical interventions Philosophies and types of PMPs Facilitating self management The clinician’s trilemma Our patients believe that they can be “fixed” Not all our patients get better Our treatments have unpredictable effects PRINCIPLES OF THERAPY AIMS Decrease pain as much as possible Increase function as much as possible Minimise adverse effects of treatment MODALITIES Psychological Physical Pharmacological Procedural PSYCHOTHERAPY PHYSICAL THERAPY PHARMACOTHERAPY PROCEDURES “Treatment” of person with chronic pain What’s happening in your world Relationships Security Work What’s happening to you as a person Reframing New learning ?Medications What’s happening to your body Exploring the body Movement ?Medications ?Procedures CLINICAL IMPROVEMENT Natural history Spontaneous symptom fluctuation Regression to the mean Sampling bias Hawthorne effect Specific effects of therapy “Non-specific” effects of therapy PLACEBO (CONTEXTUAL) EFFECT(S) Change(s) in illness attributable not to a specific pharmacological or physiological effect of a treatment but rather to the sociocultural context in which the treatment occurs PLACEBOS AND CONTEXTUAL EFFECT Contextual effect does not require a placebo Non-placebo characteristic effect + contextual effect Powerful non-placebo Weak non-placebo or placebo effect increased contextual effect decreased contextual Pharmacotherapy of Chronic Pain Ketocyclazocine Baclofen k GABAB Opioids m Ketanserin NK -1 d Clonidine 2 - Methyl - serotonin 5 - HT3 a2 Primary Afferent Fibre 5 - HT2 Glu Glu SP SP Ketamine Tricyclics AMPA GABAA NMDA Ca++ Damgo Opioids Morphine Na+ GABAA Cl- K+ d Cl- K+ Adn Midazolam Midazolam m a2 m Clonidine d K+ Adn NK - 1 K+ 5HT1B GABAB Baclofen R - Pia Neca Post Synaptic Element Unconditional, Fast and Strong. Locally adapting. PRIME Contingent, Medium speed and Medium strength. Wind - up. Adaptable, Slow Weak. Subject to inhibition by K channel activation. PRIME PHARMACOTHERAPY Non-opioid analgesics paracetamol, NSAIDs Weak µ-opioid agonists codeine, tramadol, tapentadol Strong µ-opioid agonists morphine, oxycodone, methadone, hydromorphone, fentanyl Mixed opioid ant/agonist Adjuvant analgesics buprenorphine antidepressants, anticonvulsants Finnerup et al. The evidence for pharmacological treatment of neuropathic pain. Pain 2010, 150:573-581 The “Opioid Epidemic” Australia 1990-2010 Population 29% Pharmaceutical opioid base supply 228% Per capita morphine equivalent 350mg 50 Ethics of Opioid Analgesia for Chronic Non-Cancer Pain OPIOPHILIA Patients’ right to pain OPIOPHOBIA Patients’ motivations relief Unpredictability of Sanctions on clinicians opioid-responsiveness Adverse effects, including addiction, not a problem More realistic view of addiction See also: Rich BA. Pain Clinical Updates 2007, vol XV, issue 9 Ballantyne JC, Fleisher LA. Pain 2010;148:365 Evidence for Efficacy of Opioids in Chronic Non-Cancer Pain Diversity of subjects Complexities of non-somatic influences Variability with respect to substance abuse Primary outcomes Generally poor quality Ballantyne JC, Shin NS. Efficacy of Opioids for Chronic Pain: A Review of the Evidence. Clin J Pain 2008; 24:469478 Evidence for Efficacy of Opioids in Chronic Non-Cancer Pain Extrapolation to real-life situations Risks and benefits vary over time Opioid-responsiveness always a trial Ballantyne JC, Shin NS. Efficacy of Opioids for Chronic Pain: A Review of the Evidence. Clin J Pain 2008; 24:469478 Principles of Opioid Therapy for Chronic Non-Cancer Pain 1. 2. 3. 4. 5. Comprehensive assessment Failure of adequate trial of other therapies Contractual approach to opioid usage Practical considerations Response to apparent increase in dosage requirements RACP. Prescription Opioid Policy. 2009. www.racp.edu.au/page/health-policy-and-advocacy Cohen ML, Wodak AD. Medicine Today 2010; 11:10-18 & 2012; 13:24-32 Faculty of Pain Medicine, ANZCA. Professional Document PM1, 2015. anzca.edu.au/fpm/resources/professional-documents Response To Difficulty Achieving Goals in an Opioid Trial No change in pain despite improvement in function Opioid non-responsive Unsanctioned use Comprehensive reassessment To be covered: Comprehensive assessment of patients with CNCP Managing the social and psychological dimensions Pharmacological management Opioid prescription: when and how Other biomedical interventions Philosophies and types of PMPs Facilitating self management “More studies are needed…” Shoulder pain “There is some evidence from methodologically weak trials to indicate that some physiotherapy interventions are effective for some specific shoulder disorders.” (Green et al. Cochrane Database of Systematic Reviews 2003, Issue 2. Art. No.: CD004258) Low back pain “In this systematic review, we present information relating to the effectiveness and safety of the following interventions: acupuncture, analgesics, antidepressants, back schools, behavioural therapy, electromyographic biofeedback, exercise, injections (epidural corticosteroid injections, facet joint injections, local injections), intensive multidisciplinary treatment programmes, lumbar supports, massage, muscle relaxants, non-steroidal anti-inflammatory drugs (NSAIDs), non-surgical interventional therapies (intradiscal electrothermal therapy, radiofrequency denervation), spinal manipulative therapy, surgery, traction, and transcutaneous electrical nerve stimulation (TENS).” (Chou R. Clinical Evidence [Clin Evid (Online)] 2010 Oct 08) Regarding “interventions” ? Rationale Central problem ? Evidence No sham controls ? Ethics Charging for placebo “In our opinion, withdrawal of public funding for spinal steroid injections for low back pain and/or radiculopathy should be considered on the basis of our knowledge of the placebo nature of the treatment, the costs and, not least, because of the likelihood of harm.” Harris IA, Buchbinder R. Time to reconsider steroid injections in the spine? Med J Aust 2013;199:237 “More studies [may not be] the answer…” “…the positive studies are false positives…” “No matter how many studies showed negative results, they would not persuade true believers to give up their beliefs.” Hall, H. Commentary. Pain 2011;152:711-712. To be covered: Comprehensive assessment of patients with CNCP Managing the social and psychological dimensions Pharmacological management Opioid prescription: when and how Other biomedical interventions Philosophies and types of PMPs Facilitating self management What does a good pain management program look like? Not for “pain” but a person experiencing pain (PEP) Reframes the problem By provider Of PEP Recognises the context Sociopsychobiomedical framework Interaction Respects the nervous system Allodynia Drug effects Trouble-shooting What’s happening in your patient’s world? Relationships Work Recreation What’s happening to your partient as a person? Understanding Mood ?Medications What physical treatments are you recommending? Movement ?Medications ?Procedures To be covered: Comprehensive assessment of patients with CNCP Managing the social and psychological dimensions Pharmacological management Opioid prescription: when and how Other biomedical interventions Philosophies and types of PMPs Facilitating self management Themes Complex biology of pain Sociopsychobiomedicala ssessment and management “Treatment” of person with) pain Not a “broken part” but a changed person “The body” is not the only thing (the Self-management is the aim Acute pain Chronic pain Altered nervous system Active tissue damage Changed person ALTERED ATTENTION “HYPERVIGILANCE” TRAUMA ALTERED NOCICEPTION “HYPERALGESIA” CONTEXT Relationships Security Work PERSON CNS BODY Reframing New learning ?Medications Exploring the body Movement ?Medications ?Procedures FACTORS INFLUENCING PLACEBO RESPONSES Patient expectation Conditioning Physician expertise Treatment impressive and expensive Placebo response (= response to placebo) in the experimental setting is a model for contextual effect in the clinical setting Case 1: F45 Ankle injury 2y ago: “sprained” “CRPS” diagnosed 4m later 4w inpatient PMP: physio/hydro/benzo/pregabalin/nortriptyline/opioid/int rathecal Suicidal ideation 6m later 5+w admission for (long-standing) depression: drugs/psychotherapy/TMS/ECT Personality and interpersonal issues identified… Case 1: analysis Biopsychosocial •Biomedical diagnosis (?) •One-size-fits-all approach •Medicalisation: •psychological issues •drugs/procedures •Trivial biomedical component •Why no return to work? •Delayed recognition of context Sociopsychobiomedical Case 2: F55 Fell off chair 3y ago: “lumbar sprain” Massage/“physiotherapy”/heat/TENS Palexia/Lyrica/Maxigesic “Denervation” -?repeat “Adjustment reaction with depression” Antidepressant drugs/counselling “Pain management not helpful” ALTERED ATTENTION “HYPERVIGILANCE” ALTERED NOCICEPTION “HYPERALGESIA” PAIN is one way, among many, that threats to homeostasis are signalled ALTERED ATTENTION “HYPERVIGILANCE” STRESSOR THREAT TO HOMEOSTASIS CWP ALTERED NOCICEPTION “HYPERALGESIA” Fear avoidance A behavioural response to pain characterised by a person excessively restricting involvement in activities and exercises due to heightened fear or anxiety about pain or reinjury (i.e. worry that any pain could cause tissue damage). Clinical Framework for the Delivery of Health Services TAC & WorkSafe Victoria Twin Goals Rx Injury RTW CLINICAL FRAMEWORK PRINCIPLES 1. Measure and demonstrate the effectiveness of treatment 2. Adopt a biopsychosocial approach 3. Empower the injured person to manage their injury 4. Implement goals focused on optimising function, participation and return to work 5. Base treatment on the best available research evidence CLINICAL FRAMEWORK PRINCIPLES - from a clinical perspective 1. Adopt a sociopsychobiomedical approach 2. Implement goals focused on optimising function, participation and return to work 3. Empower the injured person to manage their injury 4. Base treatment on the best available research evidence 5. Measure and demonstrate the effectiveness of management Terminology Inappropriate prescriber behaviour Unsanctioned opioid use Problematic use (patients) Illicit use (third parties) Problems Diagnosis Tolerance Hyperalgesia Pseudoaddiction (Hormonal changes) (Immune modulation) Unanswered Questions Is opioid therapy beneficial in the long term? Is there a differential effect on efficacy and safety? Is there a ceiling dose? How likely is unsanctioned use?