This adaptation in precursor responses suggests there will also b

This adaptation in precursor responses suggests there will also be adaptations in GABAergic neuroactive steroids derived from DOC. Potential role of neuroactive steroids in ethanol sensitivity and risk for alcoholism: a hypothesis While the physiological significance is unknown, dysregulation of the HPA axis is associated with ethanol dependence in humans.118,122 HPA axis suppression in alcohol dependence results in diminished

elevations of GABAergic neuroactive steroids in rodents as described above. Diminished elevations Inhibitors,research,lifescience,medical of GABAergic neuroactive steroids following ethanol exposure would result in reduced sensitivity to the anxiolytic, sedative, anticonvulsant, cognition-impairing, and discriminative stimulus properties of ethanol. Reduced sensitivity to ethanol is associated with

greater risk for the development of www.selleckchem.com/PKC.html alcoholism Inhibitors,research,lifescience,medical in individuals with alcoholism in their family131,132 Moreover, individuals with the GABAA receptor α2 subunit polymorphism that is associated with alcohol dependence exhibit substantially reduced sensitivity to the subjective effects of ethanol compared with individuals that lack this polymorphism.95 Likewise, rats and mice Inhibitors,research,lifescience,medical with low sensitivity to various behavioral effects of alcohol tend to self-administer greater amounts of ethanol in laboratory settings. The BXD recombinant inbred Inhibitors,research,lifescience,medical strains of mice, PKCγ and PKCε knockout mice, alcohol-preferring P rats, and high-alcohol-drinking (HAD) rats are but a few examples. Taken together, these observations suggest that ethanol-induced elevations of GABAergic neuroactive steroids in brain may underlie important aspects of ethanol sensitivity that may serve to prevent excessive alcohol consumption (Figure 2). The loss of these

responses Inhibitors,research,lifescience,medical may promote excessive alcohol consumption to achieve the desired effects of ethanol A deficiency in neurosteroid responses to ethanol intake could result from suppression of the HPA axis or other genetic/environmental factors that inhibit neurosteroid synthesis in brain. Hence, the lack of neurosteroid elevations in response to ethanol could underlie innate ethanol tolerance or ethanol tolerance induced by long-term ethanol use. Indeed, the observation that finasteride did much not alter the subjective effects of ethanol in subjects with the GABAA receptor a2 subunit polymorphism associated with alcohol dependence95 is consistent with the idea that neurosteroid responses contribute to ethanol sensitivity and risk for alcoholism. Both forms of tolerance may promote excessive alcohol consumption. Excessive alcohol consumption, particularly binge drinking, is a significant risk factor for all alcohol use disorders, including alcohol dependence and alcoholism. The restoration of ethanol sensitivity in ethanol-dependent patients may therefore have therapeutic utility.

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