Increased platelet responsiveness following coronary stenting : Heparin as a possible aetiological factor in stent thrombosis

Platelet activation may be a determinant of thrombotic and restenotic complications following intracoronary stenting. In order to measure the effect of stenting on platelet activation antigen expression we used whole blood flow cytometry in 18 patients undergoing Palmaz-Schatz stenting (treated with...

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Bibliographic Details
Published in:European heart journal 1998-08, Vol.19 (8), p.1239-1248
Main Authors: KNIGHT, C. J, PANESAR, M, WILSON, D. J, PATRINELI, A, CHRONOS, N, WRIGHT, C, CLARKE, D, PATEL, D, FOX, K, GOODALL, A. H
Format: Article
Language:English
Subjects:
Adenosine Diphosphate - pharmacology
Aged
Angina Pectoris - physiopathology
Angina Pectoris - therapy
Anticoagulants - adverse effects
Biological and medical sciences
Diseases of the cardiovascular system
Female
Flow Cytometry
Heparin - adverse effects
Heparin, Low-Molecular-Weight - adverse effects
Humans
Male
Medical sciences
Middle Aged
Platelet Activation - drug effects
Platelet Count
Radiotherapy. Instrumental treatment. Physiotherapy. Reeducation. Rehabilitation, orthophony, crenotherapy. Diet therapy and various other treatments (general aspects)
Stents
Thrombosis - chemically induced
Warfarin - pharmacology
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Summary:Platelet activation may be a determinant of thrombotic and restenotic complications following intracoronary stenting. In order to measure the effect of stenting on platelet activation antigen expression we used whole blood flow cytometry in 18 patients undergoing Palmaz-Schatz stenting (treated with full anticoagulation) and compared these with a group of 18 patients undergoing elective angioplasty. The effects of low molecular weight heparin and unfractionated heparin on platelet behaviour were also studied, both in vitro and in vivo to determine the contribution of prolonged heparin therapy to platelet activation following stenting. Fibrinogen binding to activated GPIIb-IIIa, and surface expression of P-selectin, GPIb and GPIIb-IIIa antigens were measured in unstimulated peripheral blood samples (rest) and on stimulation with adenosine diphosphate (0.1-10 micromol x 1(-1)) and thrombin (0.02-0.16 U x ml(-1)). No changes were seen in resting samples following angioplasty or stenting. Agonist responsiveness was unaltered after angioplasty, but in stented patients antigen expression in response to thrombin was significantly reduced (P< or =0.04), whilst the adenosine diphosphate response was significantly increased (P=0.01). Similar effects were observed in patients with unstable angina treated with either low molecular weight heparin or unfractionated heparin in vivo. In vitro, both unfractionated and low molecular weight heparin inhibited thrombin-induced platelet activation, but stimulation of adenosine diphosphate responses was more marked with unfractionated than low molecular weight heparin. There was a significant increase in platelet responsiveness to adenosine diphosphate following intracoronary stenting in patients treated with conventional anticoagulants. This was probably a consequence of treatment with heparin. Activation of platelets by heparin may explain the increased rate of stent thrombosis in patients treated with anticoagulant therapy. Low molecular weight heparins stimulate platelets less than unfractionated heparin.
ISSN:0195-668X
1522-9645
DOI:10.1053/euhj.1998.1047