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Effect of Transdermally Delivered Aspirin on Blood Coagulation Parameters

Faculty of Pharmacy, Jamia Hamdard University, New Delhi-110062, India

*Corresponding author

(Author is presently affiliated to following University)

Department of Pharmacology,

Khartoum College of Medical Sciences,

Aljerief West, Ist Block Number 398

P.O. Box 10995

Khartoum, Sudan

E-mail: areeg102@yahoo.co.in

Abstract

The efficacy of oral aspirin treatment in the secondary prevention of cardio and cerebro vascular disease is well known. However oral administration is often associated with abdominal discomfort. The feasibility of delivering aspirin transdermally from eudragit and polyvinyl acetate (PVA) matrix-type patches to enhance its antithrombotic efficiency of aspirin was investigated.  Transdermal films containing mixture of eudragit RL: eudragit RS and polyvinyl acetate were fabricated. Eudragit RL: eudragit RS (5:1) films containing 30 mg/ transdermal patch aspirin showed maximum release (11.89±1.1μg/cm²) after 24 hrs as compared to PVA films. With regards to appearance eudragit films were also wrinkle free, uniform, flexible and transparent with good adhesion property to skin.  The effect of turpentine oil and lemon oil at different concentrations on the in vitro percutaneous absorption of aspirin from eudragit copolymer patches through rat skin was investigated. Two formulation containing 50 mg/transdermal patch ASA with 0.042 ml turpentine oil and 0.042 ml lemon oil showed a significantly higher flux of ASA 4.22 mg/cm²/hr and 38.52 mg/cm²/hr respectively. The optimized formulations influenced the blood coagulation parameters (bleeding time, prothrombin time, Activated partial prothrombin time) significantly by means of affecting both the extrinsic coagulation system and the intrinsic coagulation system as compared to orally administered and control gel formulations.

Keywords:  Transdermal; Aspirin; Penetration enhancers; Antiplatelet.

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