There is optimism that advances in molecular genetics will increase our understanding of the progression from genetic susceptibility to clinically overt schizophrenia. The mainstay of managing schizophrenia at present, however, is drug therapy. Indeed, if the susceptibility gene with a required degree of predictive power can be identified, but. cannot, be modified, there is much ethical and
clinical discussion as to whether “pharmacological prophylaxis” of the potential patient, with schizophrenia with atypical neuroleptics ought to be initiated at the Inhibitors,research,lifescience,medical “prodromal” stage or even earlier. While the principles of clinical trials aimed at demonstrating the efficacy of new neuroleptic agents are relatively well established, the task of establishing their safety still remains a challenging one. This class of drugs is known to have a wide range of serious and troublesome safety problems, which include neurological, AZD5363 solubility dmso cardiac, endocrine, and metabolic side Inhibitors,research,lifescience,medical effects. Recently, developed atypical neuroleptics have succeeded in modestly reducing
these risks. The present, efficacy-orientated approach is primarily responsible for the failure of clinical trials to detect the risks that are likely to be encountered during the uncontrolled Inhibitors,research,lifescience,medical use of the drug after it is approved. The number of patients exposed is not large enough nor are all the patient subgroups likely to receive the drug during its uncontrolled clinical use Inhibitors,research,lifescience,medical represented in these preapproval clinical trials. Despite very tight, inclusion and exclusion criteria, clinical trials with neuroleptic drugs are among those with very high patient withdrawal rates. It is usually the case that the subgroups excluded from clinical trials are in fact those who are at a much greater Inhibitors,research,lifescience,medical risk. These include those patients with predisposing diseases or those receiving drugs with a potential for pharmacokinetic or pharmacodynamic interactions. Thus, the scope for detecting drug-disease or drug-drug interactions in
clinical trials is also very limited. And yet, experience has shown that these are among the most important risk factors! There are additional reasons why the safety of neuroleptic drugs should be adequately first characterized. Atypical antipsychotics have revolutionized the treatment of schizophrenia, becoming the treatment of choice for patients not only during their first, episode, but also throughout their life course. However, of particular regulatory interest, are the reports that more than 70% of prescriptions for these drugs are written for conditions other than schizophrenia, such as affective disorders (both mania and depression), autism, geriatric agitation, substance abuse disorder, senile dementia, and pathologic aggression.
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