Major Depression Clinical Trial
Official title:
Phase 4 Study of Clinical Pharmacogenomics of Antidepressant Response
The study includes two components:(1) cross-sectional (Study I), and (2) longitudinal
treatment trial (Study II). The cross-sectional component will include all subjects
initially recruited for the parent project. Genotyping characteristics will be compared with
clinical status (i.e., recovered vs symptomatic). The treatment trial component (one) will
include a subset of the subjects (n = 400) who remain significantly depressed. They will be
randomly assigned to 8-weeks of treatment with either citalopram or paroxetine. With such a
design, we wish to test the following hypotheses:
Ⅰ. Depressed patients with the short variant of the serotonin transporter (5HTTLPR) will
respond faster and better to antidepressants compared to their counterparts with the long
variant. Concurrently, patients with the 5-HTT Stin2 12/12 allele will also show better
response as compared to those with the 10/12 allele.
Ⅱ. Depressed patients who are homozygous for deficient or less active CYP2D6 or CYP2C19
enzyme(s) will be more likely to show treatment emergent side effects compared to subjects
with the wildtype alleles. Specifically, in Study II, CYP2D6 polymorphism will predict PAR
but not CIT side effects and CYP2C19 polymorphism will be associated with CIT but not PAR
side effects.
Despite remarkable progress in recent decades in modern psychopharmacotherapy, patients vary substantially in their response to antidepressants, ranging from total remission to complete treatment failure. Adverse effects, often bothersome and occasionally life-threatening, continue to represent significant challenges to patients and clinicians. Mechanisms responsible for such variability remain poorly understood. In addition, although less appreciated, substantial cross-ethnic variations in psychotropic responses often exist. Recent developments in the field of pharmacogenetics indicate that genetic factors may account for a large part of these differences in response. Specific genetic polymorphisms affecting the function of the serotonin (SERT) system has been postulated to predict the effect of antidepressants. Similarly, genetic mutations have been shown to exert a predominant influence on the expression of a number of drug-metabolizing enzymes, including most of the cytochrome P-450 enzymes (e.g., CYP2C19 and CYP3A4) that are responsible for the biotransformation of most antidepressants. Polymorphisms of genes controlling these enzymes have been found to be strongly associated with the propensity for various kinds of side effects. Capitalizing on these new developments, the proposed study will examine the predictive value of some of these genetic polymorphisms in 400 patients with DSM-IV major depression prospectively treated with citalopram (CIT). It is postulated that mutations affecting the function of SERT will predict responses to CIT, polymorphism of CYP2C19 will be associated with the side effect profiles and pharmacokinetics of CIT. The proposed study represents an extension and replication of a 5-year NIH/NIMH collaborative project that had designed and initiated in 2001 by the PI, which is currently ongoing at three sites in the U.S. ( “Ethnic Variations in Antidepressant Response” 1 R01 MH62421; 1R01MH626761R01MH62531, 07/01 - 06/06). In the original study, the inclusion of the two comparison groups, African Americans and Caucasians, whose genetic mutation patterns diverge significantly from each other, will allow us to examine how these differences affect their antidepressant response patterns and whether the associations are “replicable” across ethnicity. Results will be pooled with those derived from other sites, and will represent a rare opportunity to compare findings across Taiwanese, African American and Caucasian subjects with comparable diagnosis and treated with an identical protocol. ;
Allocation: Randomized, Endpoint Classification: Bio-equivalence Study, Intervention Model: Factorial Assignment, Masking: Open Label, Primary Purpose: Treatment
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