Acute Coronary Syndromes Clinical Trial
Official title:
Single-center Randomized Controlled Study of Omeprazole and Pantoprazole Antiplatelet Effect of Clopidogrel Clinical Randomized Controlled Trials
In order to further clarify the interaction of PPIs with clopidogrel anti - platelet effect , the investigators designed a clinical randomized controlled trials of omeprazole and pantoprazole antiplatelet effect of clopidogrel .In this experiment , the investigators have taken a randomized NSTE-ACS hospitalized patients met the inclusion criteria were randomly divided into omeprazole and pantoprazole groups . On the day of admission , all patients taking clopidogrel loading dose 300mg + aspirin 300mg and the subsequent maintenance dose of clopidogrel 75mg + aspirin 300mg and omeprazole group taking omeprazole 20mg / d , pantoprazole group taking pantoprazole 20mg / d. Respectively, on the day of admission ( before medication ) , medication for 12-24 hours , medication after 72 hours , 30 days , each taken early morning fasting venous blood again , measuring AA 、ADP - induced platelet aggregation . And selected 30 days , 6 months and 12 months to record the patient's clinical adverse events ( including death , myocardial infarction , and any revascularization , stent thrombosis , recurrent angina , rehospitalization due to cardiovascular disease , bleeding events) . To assess the impact of PPIs on clopidogrel antiplatelet effect by observing 1 year follow-up results , and further explore the optimal combination of dual anti-platelet and joint PPIs course of treatment , appropriate dosage and the best time to provide reasonable for clinical programs to create a personalized treatment system , improve the patient's quality of life .
Through a number of large-scale clinical trials , Meta analysis, and clinical treatment
guidelines confirm that clopidogrel and aspirin dual antiplatelet treatment strategies for
acute coronary syndrome (ACS) undergoing percutaneous coronary interventions(PCI) of stent
implantation surgery patients have a vital role . It can effectively suppress acute
、subacute stent thrombosis formation , reduce readmissions ratio , thus greatly improving
the quality of life of patients . A large number of clinical practice reports, although the
treatment strategies to reduce the incidence of adverse cardiovascular events ,it has
increased the possibility of the occurrence of gastrointestinal bleeding complications .
Proton pump inhibitors (PPIs) are often used to prevent gastrointestinal complications of
dual antiplatelet therapy . 2008 American College of Cardiology (ACC) / American Society of
Gastroenterology (ACG) / American Heart Association (AHA) jointly issued a consensus
document , consistently recommended that the majority of clinicians application of dual
antiplatelet and PPIs treatment for patients with risk factors for gastrointestinal bleeding
that may exist at the same time ,in order to reduce the occurrence of gastrointestinal
adverse events . But at home and abroad in recent years, there have been reports suggest
that the interaction of PPIs with clopidogrel may exist , thereby reduce the latter 's anti-
platelet effect , in order to make the incidence of adverse CV events increased about 25-64
% . In January 2009 , the U.S. Food and Drug Administration (FDA) announced a safety review
of an earlier report on the potential interaction of these two types drugs , particularly
stressed the need to carry out a large number of clinical practice research further to clear
both the interaction . PPIs antiplatelet effects of clopidogrel after PCI is not yet very
clear , clinical results on both interactions still exist many different academic
perspectives and research defects , so still need to arouse sufficient attention , continue
to carry out the relevant fields research .
In order to further clarify the interaction of PPIs with clopidogrel anti - platelet effect
, the investigators designed a clinical randomized controlled trials of omeprazole and
pantoprazole antiplatelet effect of clopidogrel .In this experiment , the investigator have
taken a randomized NSTE-ACS hospitalized patients met the inclusion criteria were randomly
divided into omeprazole and pantoprazole groups . On the day of admission , all patients
taking clopidogrel loading dose 300mg + aspirin 300mg and the subsequent maintenance dose of
clopidogrel 75mg + aspirin 300mg and omeprazole group taking omeprazole 20mg / d ,
pantoprazole group taking pantoprazole 20mg / d. Respectively, on the day of admission (
before medication ) , medication for 12-24 hours , medication after 72 hours , 30 days ,
each taken early morning fasting venous blood again , measuring AA 、ADP - induced platelet
aggregation . And selected 30 days , 6 months and 12 months to record the patient's clinical
adverse events ( including death , myocardial infarction , and any revascularization , stent
thrombosis , recurrent angina , rehospitalization due to cardiovascular disease , bleeding
events) . To assess the impact of PPIs on clopidogrel antiplatelet effect by observing 1
year follow-up results , and further explore the optimal combination of dual anti-platelet
and joint PPIs course of treatment , appropriate dosage and the best time to provide
reasonable for clinical programs to create a personalized treatment system , improve the
patient's quality of life .
;
Allocation: Randomized, Endpoint Classification: Safety Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Outcomes Assessor), Primary Purpose: Prevention
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