APC resistance and third-generation oral contraceptives: Acquired resistance to activated protein C, oral contraceptives and the risk of thromboembolic disease

doi:10.1093/humrep/16.1.3

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Human Reproduction, Vol. 16, No. 1, 3-8, January 2001
© 2001 European Society of Human Reproduction and Embryology

APC resistance and third-generation oral contraceptives

Acquired resistance to activated protein C, oral contraceptives and the risk of thromboembolic disease

Jean-Christophe Gris¹^,3, Christian Jamin², Jean-Louis Benifla², Isabelle Quere¹, Patrick Madelenat² and Pierre Mares¹

¹ Laboratoires d'Hématologie, Faculté de Pharmacie, F-34060 Montpellier et Centre Hospitalier Universitaire, F-30029 Nîmes, and ² Service de Gynécologie et Obstétrique, Hôpital Bichat, 46 rue Henri Huchard, 75018 Paris, France

Using a newly-developed technique, a severe acquired plasmaresistance to activated protein C has been described in womenusing third-generation (rather than second-generation) oralcontraceptives. The following items are discussed: (i) the technicalparameters used to appreciate the effect of activated proteinC induce a bias of interpretation, the mean intrinsic effectof activated protein C, in plasmas from women on second or third-generationoral contraceptives being strictly identical; (ii) there areno data available to show that this assay can indicate a thromboembolicrisk in asymptomatic women on oral contraceptives; and (iii)this assay is a global and non-specific test, basically sensitiveto the plasma concentrations of many coagulation factors whichare increased or decreased by oestrogens and progestogens. Forinstance protein S, in which oral contraceptive-induced modificationsaccount for the differential effect of oral contraceptives onRosing's assay, but which modifications are not related to thethromboembolic risk of oral contraceptives. The androgenic potentialof the progestogen may counteract the effect of oestrogens inthe test. More generally, in such a complex situation in whichthere is a `modification of the modification', there is no haemostasis-relatedtest which provides a risk indicator for thrombosis. Based ontesting of the plasma response to activated protein C, it isimpossible to state that third-generation oral contraceptivesinduce a more important thromboembolic risk than oral contraceptivescontaining a more androgenic progestogen.

Key words: acquired resistance/oral contraceptives/protein C/third-generation/thromboembolism

³ To whom correspondence should be addressed. E-mail: jcgris{at}chu-nimes.fr

This debate was previously published on Webtrack, www.oup.co.uk/humrep/comment—September27, 2000

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