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   influence of low-dose proton pump inhibitors administered concomitantly or separately on the anti-platelet function of clopidogrel  
   
نویسنده furuta takahisa ,sugimoto mitsushige ,kodaira chise ,nishino masafumi ,yamade mihoko ,uotani takahiro ,sahara shu ,ichikawa hitomi ,kagami takuma ,iwaizumi moriya ,hamaya yasushi ,osawa satoshi ,sugimoto ken ,umemura kazuo
منبع journal of thrombosis and thrombolysis - 2017 - دوره : 43 - شماره : 3 - صفحه:333 -342
چکیده    Proton pump inhibitors (ppis) at low doses can effectively prevent gastrointestinal bleeding due to aspirin and are widely used in japan for gastroprotection in patients taking anti-platelet agents. we examined the influence of different ppis at low doses administered concomitantly or separately on anti-platelet functions of clopidogrel. in 41 healthy japanese volunteers with different cyp2c19 genotypes who took clopidogrel 75 mg in the morning alone, or with omeprazole 10 mg, esomeprazole 10 mg, lansoprazole 15 mg, or rabeprazole 10 mg, either concomitantly in the morning or separately in the evening, we measured the inhibition of platelet aggregation (ipa, %) using verifynow p2y12 assay at 4 h after the last clopidogrel dose on day 7 of each regimen. ipa by clopidogrel with rabeprazole administered at lunchtime, approximately 4 h after clopidogrel, was also measured. mean ipas in those concomitantly receiving omeprazole, esomeprazole, lansoprazole or rabeprazole (47.2 ± 21.1%, 43.2 ± 20.2%, 46.4 ± 18.8%, and 47.3 ± 19.2%, respectively) were significantly decreased compared with those receiving clopidogrel alone (56.0%) (all ps < 0.001). this decrease was observed when ppis were administered separately in the evening. however, ipa by clopidogrel with rabeprazole administered at lunchtime was 51.6%, which was markedly similar to that of clopidogrel alone (p = 0.114). all tested ppis reduce the efficacy of clopidogrel when administered concomitantly. our preliminary data suggest that administration of rabeprazole 4 h following clopidogrel minimize potential drug–drug interactions.
کلیدواژه clopidogrel ,cyp2c19 ,platelet function ,proton pump inhibitor ,omeprazole ,esomeprazole ,lansoprazole ,rabeprazole ,drug–drug interaction ,genotype
آدرس hamamatsu university school of medicine, center for clinical research, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, department of clinical oncology, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, department of endoscopic and photodynamic medicine, japan, hamamatsu university school of medicine, first department of medicine, japan, hamamatsu university school of medicine, department of pharmacology, japan
 
     
   
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