Methadone is particularly worrisome because of its long half-life

Methadone is particularly worrisome because of its long half-life (as long as 50 hours in some patients) with unnoticed rising blood levels. In addition, methadone is known to prolong the QT interval so can lead to fatal arrhythmia (torsade de pointes). Significant sleep disturbance and sexual dysfunction can also emerge in patients

taking daily opioids. Webster et al studied 147 patients receiving daily opioids for various pain conditions and found sleep apnea in 75% (either obstructive or central).[36] Cognitive and behavioral function must be closely monitored in any patient on daily or even frequent opioid medication. Mood alteration, mental fogginess, and motivational issues are universally Panobinostat in vitro known side effects to opioids in humans. Some of these do lessen with tolerance, but symptoms of anxiety and mood change can lead to increased use. Sjogren et al in 2000 studied cognitive function in 40 patients receiving long-term oral opioid therapy for non-malignant pain, primarily sustained-release

morphine or methadone, and compared psychometric performance with 40 age-matched healthy volunteers.[37] Clear relative deficiencies in memory, attention, and psychomotor speed were found in patients on opioid therapy. However, other studies have not replicated these results. The obvious confounding issue in attempting to assess cognition and behavior is Alisertib that any abnormal function in these areas might be the result of pain, anxiety, or depression because of the medical condition rather than the opioids themselves. Along with the nearly inevitable tolerance to analgesic benefits that seems to accompany frequent opioid use, a seemingly paradoxical phenomenon – opioid induced hyperalgesia (OIH) – has been observed. This has clearly been shown to occur in many patients taking daily opioids and is diagnosed clinically by noting increased pain despite an increase in dosage (which generally happens if the prescriber incorrectly

assumes tolerance has developed). OIH, while not completely understood, probably results from a number of mechanisms including activation of excitatory anti-analgesic pathways, pain facilitation via dynorphin and CCK activation, increased activity of nociceptive pathway excitatory neuropeptides (calcitonin gene-related peptide and substance P), descending facilitation of pain involving Wilson disease protein the RVM and probably glial activation with release of cytokines that augment nociception.[38] OIH can easily be misdiagnosed as tolerance or disease-worsening, but a clue can be local allodynia, in addition heightened pain with dosage increase. Finally, as described earlier, MOH can compromise the potential benefits of opioids for relief of chronic headache disorders. With daily opioid use, presumably the risk of MOH rises significantly. While this is difficult to assess, several authors have demonstrated improvement in chronic primary headache following discontinuation of opioid medications.

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