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DOI: 10.1055/s-0038-1649849
Changes in Haemostatic Variables Induced by Oral Contraceptives Containing 50 μg or 30 μg Oestrogen: Absence of Dose-dependent Effect on PAI-1 Activity
Publication History
Received 14 November 1994
Accepted after resubmission 27 April 1995
Publication Date:
09 July 2018 (online)
Summary
Several studies have suggested a dose-response relation between the oestrogen content of oral contraceptive (OC) and the risk of both venous thrombosis and arterial disease, when oestrogen doses were higher than 50 μg. However, there is no clear epidemiological evidence for a decrease in thrombotic risk with formulations containing less than 50μg oestrogen. Therefore, we investigated haemostatic variables in users of OC containing either 30 μg (35 women) or 50μg (29 women) ethinyl estradiol as compared with non users (64 women) matched for age and smoking status. Mean values of antithrombin activity were significantly lower in 30 γg or 50 μg oestrogen users than in non users (96% and 98% vs 105%, respectively, p<0.001), but they were not significantly different between the two groups of OC users. There was a significant increase in mean values of factor VII antigen in women taking either 30μg or 50μg oestrogen as compared with non users (96% and 101% vs 85%, respectively, p<0.005). Although the difference between both groups of OC users was not significant, a positive linear trend in factor VII levels was observed within the 0-50μg oestrogen range (p <0.001). Mean levels of fibrinogen were slightly higher in 30μg or 50μg oestrogen users than in non users (2.71, 2.66 g/l vs 2.55 g/l, respectively,), but there was no significant difference between the three groups. Mean values of PAI-1 activity were significantly lower in both groups of OC users than in non users (4.89 and 4.63 AU/ml vs 6.47 AU/ml, respectively, p <0.02), but this decrease was not dose-dependent. There was no significant difference in haemostatic variables between 30 μg oestrogen preparations containing either 100μg (13 women), 150μg (3 women) or 200μg (19 women) levonorgestrel. In 50μg oestrogen preparations, the wide range of different types of progestogens did not allow valid assessment of proge- stogens effect. These data provide further evidence for an alteration of blood coagulation and fibrinolysis in OC users within the 30μg-50μg oestrogen range. However, despite a possible dose-dependent effect of oestrogen on factor VII, our results suggest no substantial change in PAI-1 activity and other markers of thrombogenic risk when oestrogen content of combined OC is decreased from 50μg to 30μg. The potential role of progestogens in haemostatic system needs further investigations.
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References
- 1 Sartwell PE, Stolley PD. Oral contraceptives and vascular disease. Epidemiol Rev 1982; 4: 95-109
- 2 Stadel BV. Oral contraceptives and cardiovascular disease. N Engl J Med 1981; 305: 612-618
- 3 Stolley PD, Strom BL, Sartwell PE. Oral contraceptives and vascular disease. Epidemiol Rev 1989; 11: 241-243
- 4 Croft P, Hannaford PC. Risk factors for acute myocardial infarction in women: evidence from the Royal College of General Practioner’s oral contraception study. Br Med J 1989; 298: 165-168
- 5 Bottiger LE, Boman G, Eklund G, Westerholm G. Oral contraceptives and thromboembolic disease: effects of lowering oestrogen content. Lancet 1980; 1: 1097-1101
- 6 Inman WH W, Vessey MP, Westerholm G. Thrombotic disease and steroidal content of oral contraceptives. A report of the committee on safety of drugs Br Med J 1970; 2: 203-209
- 7 Meade TW, Greenberg G, Thompson SG. Progestogen and cardiovascular reactions associated with oral contraceptives and comparison of the safety of 50- and 30-μg oestrogen preparation. Br Med J 1980; 280: 1157-1161
- 8 Gerstman BB, Piper JM, Tomita DK, Ferguson WJ, Stadel BV, Lundin FE. Oral contraceptive estrogen dose and the risk of deep venous thromboembolism. Am J Epidemiol 1991; 133: 32-37
- 9 La Rosa JC. The varying effects of progestins on lipid levels and cardiovascular disease. Am J Obstet 1988; 158: 1621-1629
- 10 Knopp RH. Cardiovascular effects of endogenous and exogenous sex hormones over a woman’s lifetime. Am J Obstet Gynecol 1988; 158: 1630-1643
- 11 Stampfer MJ, Willet WC, Colditz GA, Speizer FE, Hennekens CH. Past use of oral contraceptives and cardiovascular disease: A meta-analysis in the context of Nurses’ Health Study. Am J Obstet Gynecol 1990; 163: 285-291
- 12 Meade TW, Mellow S, Brozovic H, Chakrabarti RR, North RR, Haines AP, Stirling Y, Imeson JD, Thompson SG. Haemostatic function and ischaemic heart disease: principal result of Northwick Park Heart Study. Lancet 1986; 2: 533-537
- 13 Wilhemsen L, Svardsudd K, Korsan-Bengsten K, Larsson B, Welin L, Tibblin G. Fibrinogen as a risk factor for stroke and myocardial infarction. N Engl J Med 1984; 311: 501-505
- 14 Stone MC, Thorp JM. Plasma fibrinogen: a major coronary risk factor. J R Coll Gen Pract 1985; 35: 565-569
- 15 Kannel WB, Wolf PA, Castelli WP, D’Agostino RB. Fibrinogen and risk of cardiovascular disease: the Framingham Study. JAMA 1987; 13 (258) 1183-1186
- 16 Yarnell JW G, Baker IA, Sweetnam PM, Bainton D, O’Brien JR, Whitehead PJ, Elwood PC. Fibrinogen, viscosity, and white blood cell count are major risk factors for ischemic heart disease. The Caerphilly and Speedwell Collaborative Heart Disease Studies Circulation 1991; 83: 836-844
- 17 Paramo JA, Colucci M, Collen F, Van De Werf F. Plasminogen activator inhibitor in the blood of patients with coronary artery disease. Br Med J 1985; 291: 573-574
- 18 Olofsson BO, Dahlen G, Nilsson TK. Evidence for increased levels of plasminogen activator inhibitor and tissue plasminogen activator in plasma of patients with angiographically verified coronary artery disease. Eur Heart J 1989; 10: 77-82
- 19 Oseroff A, Krishna Murti C, Massett A, Tang D, Alving B. Plasminogen activator and plasminogen activator inhibitor activities in men with coronary artery disease. J Lab Clin Med 1989; 113: 88-93
- 20 Hamsten A, Wiman B, De Faire U, Blomback M. Increased plasma levels of a rapid inhibitor of tissue plasminogen activator in young survivor of myocardial infarction. N Engl J Med 1985; 313: 1557-1563
- 21 Hamsten A, De Faire U, Walldius G. et al Plasminogen activator inhibitor in plasma : risk factor for recurrent myocardial infarction. Lancet 1987; 2: 3-9
- 22 Daly L, Bonnar J. Comparative studies of 30 μg ethinyl estradiol combined with gestoden and desogestrel on blood coagulation, fibrinolysis and platelets. Am J Obstet Gynecol 1990; 163: 430-437
- 23 Quehenberger P, Kapiotis S, Partan C, Schneider B, Wenzel R, Gaiger A, Speiser W. Studies of oral contraceptives-induced changes in blood coagulation and fibrinolysis and the estrogen effect on endothelial cells. Ann Hematol 1993; 67: 33-36
- 24 Petersen K, Sildelman J, Skouby SO, Jespersen J. Effects of monophasic low-dose oral contraceptives on fibrin formation and resolution in young women. Am J Obstet Gynecol 1993; 168: 32-38
- 25 Kelleher CC. Clinical aspects of relationship between oral contraceptives and anormalities of the hemostatic system: Relation to the development of cardiovascular disease. Am J Obstet Gynecol 1990; 163: 392-395
- 26 David JL, Gaspard UJ, Gillain D, Raskinet R, Lepot MR. Haemostasis profile in women taking low dose oral contraceptives. Am J Obstet Gynecol 1990; 163: 420-423
- 27 Balleisen L, Bailey J, Epping PH, Schulte H, Van de Loo J. Epidemiological study on factor VII, factor VIII, fibrinogen in an industrial population: I. Baseline data on the relation to age, gender, body-weight, smoking, alcohol, pill using and menopause Thromb Haemost 1985; 54: 475-479
- 28 Meade TW, Haines AP, North WR S, Chakrabarti R, Howarth DJ, Stirling Y. Haemostatic, lipid and blood-pressure profiles of women on oral contraceptives containing 50 μg and 30 μg oestrogen. Lancet 1977; 2: 948-951
- 29 Poller L, Thompson JM. Clotting factors during oral contraception. Further report Br Med J 1966; 2: 23-25
- 30 Jespersen J, Kluft C. Inhibition of tissue-type plasminogen activator in plasma of women using contraceptives and in normal women during a menstrual cycle. Thromb Haemost 1986; 55: 388-389
- 31 Jerpersen J, Petersen KR, Skouby SO. Effects of newer oral contraceptives on the inhibition of coagulation and fibrinolysis in relation to dosage and type of steroid. Am J Obstet Gynecol 1990; 163: 396-403
- 32 Gram J, Munkvad S, Jespersen J. Enhanced generation and resolution of fibrin in women above the age of 30 years using oral contraceptives low in estrogen. Am J Obstet Gynecol 1990; 163: 438-442
- 33 Siegbahn A, Ruusuvaara L. Age dependence of blood fibrinolytic components and the effects of low-dose oral contraceptives on coagulation and fibrinolysis in teenagers. Thromb Haemost 1988; 60: 361-364
- 34 Egeberg O. Inherited antithrombin deficiency causing thrombophilia. Thromb Diathes Haemorrh 1965; 13: 516-530
- 35 Conard J, Cazenave B, Samama M, Horellou MH, Zorn JR, Neau C. AT III content and antithrombin activity in oestrogen-progestogen and progestogen-only treated women. Thromb Res 1980; 18: 675-681
- 36 Sabra A, Bonnar J. Haemostatic system changes induced by 50 |ig and 30 |xg estrogen/progestogen oral contraceptives. Modification of oestrogen effects by levonorgestrel. J Reprod Med 1983; 28 suppl 85-91
- 37 Eriksson E, Ranby M, Gyzander E, Risberg B. Determination of plasminogen inhibitor in plasma using t-PA and a chromogenic single-point poly-d-lysin stimulated assay. Thromb Res 1988; 50: 91-101
- 38 Odegaard OR, Lie H, Abildgaard U. Heparin cofactor activity measured with a amidolytic method. Thromb Res 1975; 6: 28
- 39 Clauss A. Gerinnungsphysiologische Schnellmethode zur Bestimmung des Fibrinogens. Acta Haematol 1957; 17: 237-46
- 40 Boyer C, Wolf M, Rothschild C, Migaud M, Amiral J, Manucci PM, Meyer D, Larrieu MJ. An enzyme immunoassay (ELISA) for the quantitation of human factor VII. Thromb Haemost 1986; 56: 250-255
- 41 Scarabin PY, Van Dreden P, Bonithon-Koop C, Orssaud G, Bara L, Conard J, Samama M. Age-related changes in factor VII activation in healthy women. Clin Sci 1988; 75: 341-343
- 42 Campbell SJ, Mackie IJ, Robinson GE, Machin SJ. Contact factor mediated fibrinolysis is increased by the combined oral contraceptive pill. Br J Obst Gynecol 1993; 100: 79-84
- 43 Juhan-Vague I, Alessi MC, Joly P, Thirion X, Vague P, Declerck PJ, Serradimigni A, Collen D. Plasma plasminogen activator inhibitor 1 in angina pectoris. Influence of plasma insulin and acute-phase response Arteriosclerosis 1989; 9: 362-367
- 44 Juhan-Vague I, Alessi MC. Plasminogen activator inhibitor 1 and atherothrom- bosis. Thromb Haemost 1993; 70: 138-143
- 45 Kooistra T, Bosma PJ, Jepersen J, Kluft C. Study of the mechanism of action of oral contraceptives with regard to fibrinolytic variables. Am J Obstet Gynecol 1990; 163: 404-412
- 46 Scarabin PY, Bara L, Samama M, Orssaud G. Further evidence that activated factor VII is related to plasma lipids. Br J Haematol 1985; 59: 91-101
- 47 Miller GJ, Walter SJ, Stirling Y, Thompson SG, Esnouf MP, Meade TW. Assay of factor VII activity by two techniques: evidence for increased conversion of VII to a-Vila in hyperlipidemia, with possible implications for ischaemic heart disease. Br J Haematol 1985; 59: 249-258
- 48 Plu-Bureau G, Scarabin PY, Bara L, Malmejac A, Guize L, Samama M. Factor VII activation and oral contraceptives. Thromb Res 1993; 70: 275-280
- 49 Morrissey JH, Macik G, Neuenschwander PF, Comp PC. Quantitation of actived factor VII levels in plasma using a tissue factor mutant selectively deficient in promoting factor VII activation. Blood 1993; 81: 734-744