A comparative study to evaluate the cardiovascular risk of selective and nonselective cyclooxygenase inhibitors (COX-Is) in arthritic patients

Uma A. Bhosale; Nilofar Quraishi; Radha Yegnanarayan; Dileep Devasthale

doi:10.1515/jbcpp-2014-0005

Artikel

A comparative study to evaluate the cardiovascular risk of selective and nonselective cyclooxygenase inhibitors (COX-Is) in arthritic patients

Uma A. Bhosale , Nilofar Quraishi , Radha Yegnanarayan und Dileep Devasthale

Veröffentlicht/Copyright: 12. März 2014

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Aus der Zeitschrift Journal of Basic and Clinical Physiology and Pharmacology Band 26 Heft 1

Abstract

Background: During the past 2 years, a great deal of evaluation has been accomplished on the cardiovascular (CV) effects of nonsteroidal anti-inflammatory drugs (NSAIDs), nonselective and selective cyclooxygenase-2 inhibitors (COX-2-Is). Clinical trial databases for nonselective and selective COX-2-Is have shown variable effects on CV risk. There is much controversy regarding the CV safety of these selective and nonselective COX inhibitors (COX-Is). This study was therefore conducted to assess and compare the CV risk of COX-Is in arthritic patients over a period of time.

Methods: In this prospective comparative study, adult arthritics of either sex who were freshly diagnosed or taking COX-Is for <3 months were included. Patients were grouped into nonselective and selective COX-2-I groups with reference to the treatment they received, whereas arthritics with no history of COX-I treatment were included as controls. CV risk factors like blood pressure (BP), blood sugar level (BSL), lipid profile, and body mass index (BMI) were assessed and compared; the demography of CV risk factors was also studied. Data obtained were analyzed with Student’s t-test using OpenEpi statistical software (Andrew G. Dean and Kevin M. Sullivan, Atlanta, GA, USA).

Results: The study clearly revealed that all NSAIDs exhibit potential CV risk; however, selective COX-2-Is were found to exhibit more CV risk. BMI, BP and lipid profile, the potential CV risk factors, showed significant impairment in a selective COX-2-I group: p<0.01, p<0.001 and p<0.05, respectively, vs. baseline and p<0.05 for BMI and triglycerides vs. nonselective COX-Is.

Conclusions: This study depicts the impending CV risk of selective COX-2-Is and confirms and reevaluates the results of earlier studies in this regard.

Keywords: body mass index; cardiovascular risk; cyclooxygenase inhibitors; lipid profile

Corresponding author: Dr. Uma A. Bhosale, Professor, Department of Pharmacology, Smt. Kashibai Navale Medical College and General Hospital, Narhe (Ambegaon), Pune-411041, Maharashtra, India, Phone: 020-24106148, Fax: 020-24106148, Mobile: 09226767554, E-mail: umabhosale2000@gmail.com

Acknowledgments

The authors are thankful to Dr. A.V. Bhore, Dean, Smt. Kashibai Navale Medical College (SKNMC), Dr. Madhav Khadilkar, Head of Department (HOD) Orthopaedics, and Dr. Dnyaneshwari Ghadage Central Clinical Laboratory (CCL) in-charge (I/C) for providing facilities to carry out the experiments in this work.

Conflict of interest statement

Authors’ conflict of interest disclosure: The authors stated that there are no conflicts of interest regarding the publication of this article.

Research funding: None declared.

Employment or leadership: None declared.

Honorarium: None declared.

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Received: 2014-1-11

Accepted: 2014-2-8

Published Online: 2014-3-12

Published in Print: 2015-1-1

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Artikel in diesem Heft

https://doi.org/10.1515/jbcpp-2014-0005

Schlagwörter für diesen Artikel

body mass index; cardiovascular risk; cyclooxygenase inhibitors; lipid profile