Hypothesizing that Putative Dopaminergic, Melatonin, BenzodiazepineReward Circuitry Receptor(s) Activator Provides Sleep Induction Benefits
2014
The issue of insomnia is a global phenomenon which requires additional in-depth research. Insomnia especially
in alcohol-dependent patients, for example, may lead to suicide. It is noteworthy that childhood sleep problems
predict the onset of drinking in boys. We now know that while there are multi-faceted reasons for sleep problems
and disturbances (e.g. sleep drive homeostasis, circadian rhythm physiology, and genetic influences), the scientific
community has not been able to deliver an appropriate solution. Some benefit has been noted with cognitive
behavioral therapy, but it has minimal effects in patients relapsing from drugs especially alcohol, cocaine and
opiates. While there are a number of pharmaceutical drugs developed to treat insomnia, most have associated
side effects and even addiction liability. We do know that benzodiazepines hijack the midbrain dopamine system
leading to addiction. Finally, it has been proposed that dopamine D2 receptors are involved in rapid eye movement
sleep, suggesting as proposed herein that dopaminergic activation is a worthwhile mechanism to explore in the
future. The concepts presented herein on potential nutrigenomic therapy warrants further in-depth analysis. In this
regard we hypothesize based on both literature review and empirical data that a putative dopaminergic, melatonin,
benzodiazepine reward circuitry receptor(s) activator provides sleep induction benefits.
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