Genetic Determinants of CYP2C19 Gene *2 and *3 Loss of Function Alleles
and Response to Anti Platelet Therapy (Clopidogrel) and Cardiovascular
Events. (A Study in Kashmir, North India)

Irfan Ahmad Bhat; Arshad A. P; ith; Irfan Yaqoob; Shehjar Faheem; Imran Hafeez; Jahangir R Beig; Zafar A. Shah; Khurshed Iqbal

doi:10.4172/0974-8369.1000258

Awards Nomination 20+ Million Readerbase

Google Scholar citation report

Citations : 3988

Biology and Medicine received 3988 citations as per Google Scholar report

Biology and Medicine peer review process verified at publons

25+ Million Website Visitors

Indexed In

Open J Gate
Genamics JournalSeek
CiteFactor
Cosmos IF
Scimago
Ulrich's Periodicals Directory
Electronic Journals Library
RefSeek
Hamdard University
EBSCO A-Z
Directory of Abstract Indexing for Journals
OCLC- WorldCat
Proquest Summons
Scholarsteer
ROAD
Virtual Library of Biology (vifabio)
Publons
Geneva Foundation for Medical Education and Research
Google Scholar

Useful Links

Share This Page

Journal Flyer

Tweets by biology_med

Open Access Journals

Abstract

Genetic Determinants of CYP2C19 Gene 2 and 3 Loss of Function Alleles and Response to Anti Platelet Therapy (Clopidogrel) and Cardiovascular Events. (A Study in Kashmir, North India)

Irfan Ahmad Bhat, Arshad A. Pandith, Irfan Yaqoob, Shehjar Faheem, Imran Hafeez, Jahangir R Beig, Zafar A. Shah and Khurshed Iqbal

Background: Studies have demonstrated that the mutant *2 and*3 allele of the CYP2C19 loss-of-function polymorphism is associated with diminished metabolization of clopidogrel and an attenuated platelet response to clopidogrel treatment. Since no such study has been conducted in this region, we examined CYP2C19 polymorphism in Acute Coronary Syndrome (ACS) patients on clopidogrel treatment, and its effect on the cardiovascular outcomes.
Material and Methods: A total of 100 samples of ACS were included in this study and genotyping of CYP2C19 *2 and *3 gene polymorphisms was performed by a Polymerase chain reaction-Restriction fragment length polymorphism (PCR-RFLP).
Results: The distribution of CYP2C19*2 allele wild *1/*1, Heterozygous *1/*2 and homozygous mutant *2/*2 genotypes was 56%, 34% and 10% respectively while for CYP2C19*3 wild*1/*1 and heterozygous *1/*3 genotypes was 84% and 16% respectively. The frequency of compound heterozygotes (*2/*3) was found in 9% (9 of 100 patients). CYP2C19 *1/*2 allele was found in 03 of 34 (8.8%) patients who had CV events followed by 2 of 10 (20%) patients with mutant genotype CYP2C19*2 (*2/*2) on follow up. In the CYP2C19*3, 31.2% having heterozygous genotype (*1/*3) had CV events as compared to 11.9% with *1/*1 (31% v/s 11.9% p> 0 .05). In the poor-metabolizer group (*2/*2 or *2/*3), 20.1% of patients had CV events on follow up compared to 15.6% in the extensive metabolizer group (*1/*1), whereas in the intermediate group only 10% of patients had CV events (p>0.05).
Conclusion: We conclude that patients carrying CYP2C19 loss-of-function alleles had a higher rate of subsequent cardiovascular events than as against those with normal allele. Lack of significant events even in presence of variant alleles justifies us to some extent to continue clopidogrel in our patients

Biology and Medicine