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Hypnotics and OSA: Rumors and Facts DOUGLAS KIRSCH, MD CLINICAL INSTRUCTOR, HARVARD MEDICAL SCHOOL REGIONAL MEDICAL DIRECTOR, SLEEP HEALTHCENTERS Purpose of This Talk To examine the question of whether hypnotics are dangerous in patients who have untreated sleepdisordered breathing To review information about whether some hypnotics may be beneficial in the treatment of OSA To Cover: A Case What are Hypnotics Used For? What are Hypnotics? Do Hypnotics Affect the Airway? Can Hypnotics be of Benefit in OSA Treatment? Close A Case An Early Case (1981) A 38-year-old man with a long-standing history of insomnia and daytime sleepiness was evaluated. He was found to have 7-18 primarily obstructive apneas per night on four baseline recordings. On the first two nights on which he received 30 mg of the benzodiazepine hypnotic flurazepam, there were 22 and 100 apneas, and during the daytime he became extremely sleepy. Mendelson WB, Garnett D, Gillin JC. J Nerv Ment Dis. 1981 Apr;169(4):261-4 An Early Case, Part II Upon cessation of medication, his clinical condition improved, and the number of apneas decreased to 11 and 6 on withdrawal nights 4 and 6. Although respiratory depression is neither invariable nor unique to flurazepam, this case suggests that it may be a clinically significant problem with recommended oral doses in some individuals Mendelson WB, Garnett D, Gillin JC. J Nerv Ment Dis. 1981 Apr;169(4):261-4 Why Use a Hypnotic? What is Insomnia? Insomnia is a symptom: Difficulty in sleep initiation “ I can’t fall asleep” Difficulty in sleep maintenance “I keep waking up all night” Complaint of non-restorative sleep “I just don’t feel rested in the morning” Epidemiology of Insomnia NSF Poll 2005 54% reported that, within the past year, they have experienced at least one symptom of insomnia at least a few nights a week 33% said they have experienced at least one symptom every night or almost every night. Symptoms (at least a few times per week) Waking up feeling unrefreshed (38%) Waking up a lot during the night (32%) Difficulty falling asleep (21%) Waking up too early and not able to get back to sleep (21%) Hypnotics Benzodiazepines Lorazepam, Diazepam, Clonazepam, etc. Non-Benzodiazepine Receptor Agonists Zolpidem, Eszopiclone, Zaleplon Others: Alcohol Antidepressants: trazadone Anti-histamines: diphenhydramine Anti-psychotics: quietapine Sodium Oxybate http://belaray.com/blog/wp-content/uploads/2008/06/medication.jpg Insomnia Medications Wilson and Nutt, Clin Med 2005 Sleeping Medications: General Rules Treatment with medications should: begin with the lowest possible effective dose be short-term, if used nightly be intermittent, if used long-term be used only in combination with good sleep practices and/or behavioral approaches Practice Parameters, AASM Hypnotics: A Survey of 130 Patients Lu et al. JCSM 2007 Prescription Sedatives in OSA Pts. Sleep specialists tend to prescribe sedatives at a lower rate for patients with OSA than nonsleep specialists Lu et al. JCSM 2007 Benzodiazepines The “older” class of sleeping aids They are considered “CNS depressants” Enhancement of the effect of the neurotransmitter GABA Also used to treat anxiety, insomnia, agitation, seizures, muscle spasms, alcohol withdrawal 100 million scripts written in 1999 (DEA) http://en.wikipedia.org/wiki/Benzodiazepine http://library.thinkquest.org/C0115926/drugs/sedative2.htm Changes in Sleep with Benzos: Meta-analysis Nowell et al., JAMA, 278:24, 1997 Another Benefit of Hypnotics? Sedatives and Falls In 34,163 nursing home residents (76% women, mean age 84 +/- 8 y) Evaluated Hypnotic use Hypnotics as defined by CMS included aprobarbital, flurazepam, quazepam, triazolam, pentobarbital, ethchlorvynol, estazolam, temazepam and secobarbital; others such as NBZRAs (e.g., zolpidem) were also included Hypnotic use did not predict falls (adjusted odds ratio (AOR) 1.13, 95% confidence interval (CI) 0.98, 1.30). In contrast, insomnia did predict future falls (AOR 1.52, 95% CI 1.38, 1.66). J Am Geriatr Soc 53:955–962, 2005 A Hypnotic Risk: MVAs in OSA Lu et al. JCSM 2007 Early Studies with Benzodiazepines and Sleep http://thebrain.mcgill.ca/flash/i/i_04/i_04_m/i_04_m_peu/i_04_m_peu.html COPD Chronic Obstructive Pulmonary Disease Chronic obstructive bronchitis and emphysema a pair of two commonly co-existing diseases of the lungs in which the airways become narrowed Associated with symptoms such as dyspnea, cough and sputum production. COPD is caused by noxious particles or gas, most commonly from tobacco smoking, which triggers an abnormal inflammatory response in the lung http://en.wikipedia.org/wiki/COPD COPD and Benzodiazepines In 1972, Gaddie et al Nitrazepam 10mg may cause hypoventilation in 6 pts. with COPD Ex: 1 Pt: PaO2 fell from 48 to 35 mm Hg while the PaCO2 tension rose from 59.5 to 68 mm Hg Clark et al (1971) and Model (1973) Reported serious benzodiazepine-induced respiratory depression in patients with COPD March 2, 1990 The American Journal of Medicine Volume 88 (suppl 3A) What is Hypoventilation? Hypoventilation is too shallow or too slow breathing, which does not meet the needs of the body. It may also refer to reduced lung function. If a person hypoventilates, the body's carbon dioxide level rises, which results in too little oxygen in the blood. CO2 O2 Shea SA, White DP. Disorders of ventilatory control. In: Goldman L, Ausiello D, eds. Cecil Medicine. 23rd ed. Philadelphia, Pa: Saunders; 2007:chap 86 http://www.nlm.nih.gov/medlineplus/ency/article/002377.htm http://www.southdartmoor.devon.sch.uk/pe/1127505986415.internal_lungs260.gif What is Hypoventilation (PSG)? CO2 >44 & O2 < 88 http://img.medscape.com/fullsize/migrated/491/438/sin491438.fig2.gif Why Does Hypoventilation Occur? Benzodiazepines may depress the arousal response to hypoxia and hypercapnia during sleep and reduce genioglossal muscle tone So what does that mean for an OSA patient? Hedemark LL, Kronenberg RS. Flurazepam attenuates the arousal response to co2 during sleep in normal subjects. Am Rev Respir Dis 1983;128:980-3. Normal System for an OSA patient Airway Collapse ↑ Carbon Dioxide Levels ↓ Oxygen levels Arousal System with Benzodiazepines Airway Collapse + ↓ Oxygen levels Benzos Arousal ↑ Carbon Dioxide Levels Hypnotics and The Airway http://content.revolutionhealth.com/contentimages/n1573.jpg Diazepam Injection in a Cat 150 100 (% control) Peak Integrated activity Phrenic Nerve Output Hypoglossal Nerve Output 50 Diazepam Injection 0 0 5 15 30 Minutes after injection 60 Sanders MH. In: Principles and Practice of Sleep Medicine. Philadelphia: W.B. Saunders Company, 1994. Benzos and the Airway Benzos may reduce genioglossal muscle tone http://www.pwsdots.org/uploads/osa.jpg Summary: Pathophysiology of OSA Awake: Small airway + neuromuscular compensation Loss of neuromuscular compensation Sleep Onset + Decreased pharyngeal muscle activity Airway collapses Hyperventilate: connect hypoxia & hypercapnia Airway opens Benzos Pharyngeal muscle activity restored Apnea Hypoxia & Hypercapnia Increased ventilatory effort Arousal from sleep Alcohol, Apnea, and the Airway Alcohol as a Sleep Aid? • Alcohol is also used as a sleep aid • 28% of insomniacs indicated that they had used alcohol to help them fall asleep • Occasional insomniacs used alcohol for an average of 3.6 nights/month • Chronic insomniacs used alcohol for an average of 6.8 nights/month. • An equal number of occasional insomniacs and chronic insomniacs (67%) described alcohol as an effective or very effective method to induce sleep. Ancoli-Israel S, Roth T. Sleep. 1999;22(suppl 2):S347-S353. Risk Factor: Alcohol Before Alcohol Phrenic Hypoglossal Blood Alcohol = 83 mg/dl Phrenic Hypoglossal Blood Alcohol = 134 mg/dl Phrenic Hypoglossal Bonara M et al. Am Rev Respir Dis 1984;130 © American Lung Association. A Fun Study? (i.e., 1982 Studies) Evaluating the effect of alcohol on sleep-disordered breathing. On the night after the control study, (6.00-9.00 pm) the subject drank wine or beer under supervision, to an amount equivalent to the maximum he would drink on social occasions. Issa and Sullivan, JNNP 1982 http://www.brainandspinalcord.org/blog/wp-content/uploads/2009/10/alcohol.jpg OSA Patient, Control Night; ex: Hour 1 Diaphragmatic EMG Issa and Sullivan, JNNP 1982 OSA Patient, Alcohol night; ex. Hr 1 Prolonged Apneas and worse Oxygen Desaturations with Alcohol Issa and Sullivan, JNNP 1982 OSA Patient A B A) OSA patient, Control night B) Same patient, Alcohol night Issa and Sullivan, JNNP 1982 What about non-OSA?: A Snoring Patient A B A) Snoring patient, Control night B) Same patient, Alcohol night Issa and Sullivan, JNNP 1982 Results of this Alcohol Study In all 7 pts. studied, alcohol exacerbated the sleep-induced breathing abnormalities, and variably caused worsening of SaO2 in sleep. The effects of alcohol were: Dose related Occurred during the first 1-2 hr of sleep following alcohol intake. The finding was that alcohol intake can induce OSA in subjects with “benign chronic snoring”. 1) Alcohol clearly increased the duration of apneic episodes 2) It promotes upper airway occlusion during sleep Issa and Sullivan, JNNP 1982 Does Alcohol Cause Other Problems? Healthy Elderly Subjects 0.6mg/kg ethyl alcohol (whiskey) 1h before bed In case of alcohol: Those patients with initial AHI of 5-10 -> increased apneas 1 patient had increased PVCs with apneas Guilleminault et al, Journal of Gerontology 1984 39(6):655-661 Alcohol and CPAP Ten obese male subjects undergoing CPAP 1st night – CPAP titration 2nd night – Control night at correct PAP pressure 3rd night - subjects ingested either 1.5 (A) or 2 (B) ml/kg of 50 percent ethanol (100 proof vodka) over one half-hour starting 1 h before bedtime. If using CPAP No Change with Alcohol Chest 1991: 99:339-43) Review: Effects of Alcohol The genioglossus and geniohyoid muscles undergo a decrease in tone during REM sleep Alcohol, which depresses the CNS, significantly decreases the activity of the genioglossus muscle during sleep and may be a factor in snoring (partial obstruction of the upper airway) or OSA (complete upper airway obstruction). However, alcohol with PAP in place does not have as much of an effect on AHI Guilleminault, The American Journal of Medicine Volume 88 (suppl 3A); March 2, 1990 So, What Happens with Benzos and OSA? http://www.americasleeps.com/_borders/Snoring1.jpg Effect of 30 mg of Flurazepam, 1982 Double-blind, placebo-controlled, randomized study 20 patient, 17 men and 3 women In controls, SDB minimally worse with 30 mg Flurazepam FLURAZEPAM AND NOCTURNAL OXYGEN DESATURATION-DOLLY AND BLOCK, AJM 1982 Flurazepam in Controls In these patients, flurazepam had the same effect as alcohol, i.e., a complete airway obstruction was noted compared with baseline. http://www.21stcenturydental.com/smith/sleepapena_tapappliance.htm Berry, 1995: Triazolam and OSA Assessment of the effect of triazolam (0.25 mg) on apnea duration and the arousal response to airway occlusion during sleep in patients with severe OSA. 12 male subjects were studied on two nights Mean age of 46.6 +/- 14.1 yr Mean weight of 260.8 +/- 55.9 lb They ingested triazolam (0.25 mg) or placebo 0.5h before bedtime in a randomized double-blind crossover manner. Berry RB, Kouchi K, Bower J, Prosise G, Light RW Am J Respir Crit Care Med. 1995 Feb;151(2 Pt 1):450-4. Berry, 1995: Triazolam and OSA In non-rapid-eye-movement (NREM) sleep Mean duration of event was slightly increased with drug: Seconds: Mean nadir in SaO2 lower on drug nights % 26.8 vs 23.8, p < 0.02 Saturation: 80.1 vs 84.2, p < 0.001 In NREM sleep, the deflections in esophageal pressure prior to apnea termination were higher on triazolam nights Pes: 53.3 vs 44.5 cm H2O, p < 0.001 Triazolam increases the arousal threshold to airway occlusion This results in only modest prolongation of event duration and increased desaturation at a dose of 0.25 mg in a group of OSA pts. Berry RB, Kouchi K, Bower J, Prosise G, Light RW Am J Respir Crit Care Med. 1995 Feb;151(2 Pt 1):450-4. Nitrazepam in OSA patients 14 consecutive patients (12 males and 2 females), found to have mild to moderate OSA (60–180 apneas/6 h of self-reported sleep time) The principal finding of this study was that NIT had no consistent effect on the severity of sleep-disordered breathing in patients with mild to moderate SA. Eur Respir J, 1994, Berry, 1992: Triazolam and Arousals 6 men, mean age 28.1 +/- 7.1 yr , had their arousal response tested by occluding a mask covering the nose with the mouth sealed. They ingested triazolam (0.25 mg) or placebo one-half hour before bedtime in a randomized double-blind crossover manner. Mask occlusion was performed 1-4 h after triazolam/placebo ingestion while the subjects breathed air /O2 mix -> SaO2 of 98%. Results The time to arousal was significantly longer on triazolam nights (32.0 +/- 5.2 s versus 22.6 +/- 3.2 s, p < 0.01). Conclusion: triazolam prolongs the time to arousal following airway occlusion by increasing the arousal threshold. Berry RB, McCasland CR, Light RW. Am Rev Respir Dis. 1992 Nov;146(5 Pt 1):1256-60. Newer Hypnotics: Are They Better? http://www.nytimes.com/2004/11/14/business/yourmoney/14drug.html?_r=1 Kryger, 2007: Ramelteon and OSA Ramelteon is a selective MT(1)/MT(2)-receptor agonist indicated for insomnia Double-blind, randomized, crossover study 26 adults with mild to moderate OSA received ramelteon 16 mg and placebo for one night each, administered 30 min before habitual bedtime. AHI was similar: 11.4 vs 11.1, P = 0.812 Ramelteon – no effect on # of central, obstructive, or mixed apneas. No significant differences were observed in SaO(2) for the entire night (95.1 vs 94.7%); P = 0.070 Ramelteon did not statistically affect sleep when evaluated by polysomnography and post-sleep questionnaire. Kryger M, Wang-Weigand S, Roth T. Sleep Breath. 2007 Sep;11(3):159-64.. Rosenberg, 2007: Eszopiclone and OSA This double-blind, randomized crossover study Patients (35–64 yrs) with mild-to-moderate OSAS [AHI 10-40]. Patients received eszopiclone 3 mg or placebo for two consecutive nights Results Mean total AHI, was similar to placebo - 16.5 (plac) and 16.7 (esz) No significant differences in respiratory arousals, duration of respiratory episodes, or oxygen saturation were noted. Significant differences in: Sleep efficiency (85.1% and 88.4%) Wake time after sleep onset (61.8 and 48.1 min) Wake time during sleep (55.9 and 43.2 min). Rosenberg R, Roach JM, Scharf M, Amato DA. Sleep Med. 2007 Aug;8(5):464-70. 2007 Zaleplon and OSA on PAP Placebo controlled cross-over design: 15 mild to moderate OSA patients for the presence of worsening apnea with home-monitoring Administering zaleplon (10 mg) or Placebo over a period of five consecutive nights then cross over Results: No statistically significant treatment differences between zaleplon and placebo were observed AHI (ZN=7.2 vs PL=7.5; p=0.602) Mean SpO2 (ZN=94.6 vs PL=94.7; p=0.859). Small difference: ZN (79.2±1.3) and PL (82.1±0.9) for nadir SpO2 (p=0.008). These data support the hypothesis that short-acting, non-benzodiazepines may be used safely in middle-aged patients with mild to moderate OSA while receiving CPAP therapy in the home environment. Coyle et al. JCSM 2005 Effect of Zolpidem vs. Flurazepam In this 1988 study, Zolpidem was associated with slightly higher AHI and lower oxygen saturations than Flurazepam or placebo. However, the n was 12 patients Pharmacol Biochem Behav. 1988 Zolpidem and OSA on PAP Obese adult patients who had been undergoing treatment of severe OSA (AHI > 30/hour) with CPAP therapy for least 6 months. All patients were compliant with their CPAP therapy 14 men and 2 women 3 nights: Titration, and then the patient slept in the lab with PAP and one night of placebo and one night of zolpidem 10 mg in a randomized order Berry, Sleep 2006 Berry, Sleep 2006: Respiration There was no significant effect of zolpidem on any respiratory variable Berry, Sleep 2006: AHI The AHI overall, AHI during REM sleep, and the AHI during supine sleep did not differ between placebo and zolpidem nights. In summary, in a study of 16 patients with severe OSA, there was no significant worsening in the AHI or in any index of arterial oxygen desaturation during CPAP treatment with the acute use of zolpidem, 10 mg. Patients Often Feel Trapped By PAP Can Hypnotics Help This process? http://uashome.alaska.edu/~jndfg20/website/youngfrankenstein.gif Benefits to Sedatives in Sleep Apnea? Tolerance to CPAP can be problematic for patients Ranges of 50-70% of continued use over time The only consistently reliable predictor of long-term adherence has been the use of CPAP during the initial treatment period Long term adherence patterns may be determined within the first few days of therapy. Therefore, strategies aimed at improving adherence with therapy should focus on the initial experience with CPAP Methods to Improve CPAP tolerance Adjustment through continued use For those experiencing difficulty: Early Education Alterations in mask Changing pressures / type of pressure delivery Humidification Sedatives? Can Hypnotics Help with PAP? So, CPAP is hard to use, particularly if poorly tolerated early. Can the addition of a hypnotic medication help improve PAP tolerance? Bradshaw, Chest 2006 Evaluation of Zolpidem 10mg vs. Placebo during initiation of PAP Will it help improve PAP use over 28 days? Bradshaw, Chest 2006: Study Flow CHEST 2006; 130:1369–1376 Bradshaw, Chest 2006: Results in CPAP CHEST 2006; 130:1369–1376 Use of Eszopiclone in Polysomnography Prospective, double-blinded, randomized, placebo- controlled trial assessing the effect of eszopiclone 3 mg on the quality of polysomnography 3 study arms: diagnostic polysomnography, split-night polysomnography, and CPAP titration polysomnography 79 diagnostic studies, 67 split-night studies, and 80 CPAP titration studies Enrolled 226 subjects: 113 received eszopiclone and 113 received placebo Letteri, Sleep 2008 Letteri, Sleep 2008 Non-usable polysomnograms were defined as studies with less than 120 min of total sleep time (does not meet criteria for a diagnostic study) or complete CPAP intolerance. Poor quality polysomnograms were defined as studies with less than 120 min of TST, sleep efficiency less than or equal to 70%, or an incomplete CPAP titration. Defined incomplete CPAP titrations as those with a residual AHI ≥ 5 on the highest level of CPAP achieved, or complete CPAP intolerance. CPAP intolerance was defined as the patient’s complete inability to sleep on CPAP or their request to end the study prematurely due to CPAP discomfort. Letteri, Sleep 2008 Individuals were not studied both with and without this agent. Therefore, the study does not directly address the question of whether or not eszopiclone has these effects in individual patients. Letteri, Sleep 2008 Letteri, Annals Int Med 2009 Evaluation of Eszopiclone to improve CPAP use for 14 days with open label afterward Letteri, Annals Int Med 2009: AEs Letteri, Annals Int Med 2009: Effect on PAP Finally, One Last Point We’ve reviewed that data that hypnotics may help with PAP use, but… Can “hypnotic” medications actually treat OSA? Sodium Oxybate and OSA OSAS pts. (n=48) off treatment received 2-week SXB or placebo (PBO) treatment with PSG at baseline and day 14. SXB led to a reduction in mean AHI with SXB and significantly increased slow wave sleep duration (5.2± 25.0 min vs. 29.4±37.0 min; p=0.0038). George et al., Sleep Breathing Jan 2010 Summary Data is MIXED Data suggests that alcohol and benzodiazepines may worsen sleep disordered breathing in patients who already are at risk for it Some studies demonstrate that use of NBZRAs may be useful in CPAP titration and early home PAP use