ORAL CONTRACEPTION AND REPLACEMENT THERAPY - THE SIGNIFICANCE OF THE PROGESTOGEN FOR CARDIOVASCULAR-DISEASES

Epidemiological data have demonstrated, that the progestogen component of oral contraceptives is involved in the development of hypertension, ischaemic heart diseases and stroke. It had been suggested, that atherosclerotic lesions due to the unfavourable effect on lipid metabolism of progestogens with androgenic properties, play a causal role. It has, however, been shown, that there is no development of atherosclerosis despite reduced HDL and elevated LDL, presumably because of the induction of hepatic LDL- and remnant-receptors by the strong effect of ethinyl-oestradiol upon the liver. A series of experimental and clinical findings indicates that vasospasms caused by the vasoconstrictory effect of progestogens are involved in the development of arterial thromboses. In postmenopausal women, the additional administration of progestogens to the oestrogen treatment may trigger ischaemic diseases, particularly in the presence of vascular lesions. Oestrogens exercise a pronounced vasodilatory effect and stabilize the vascular tonus - through changes in the responsiveness of endothelium and smooth muscle cells to vasoactive compounds, through modulation of neurotransmitter release from nerve endings, and through direct blocking of calcium channels. The effects depend essentially on an intact endothelium. By a direct action on the vascular wall, progestogens increase the sensitivity of arteries to vasoconstrictory compounds and reduce blood flow. As aldosterone increases the number of beta-adrenergic receptors in the arterial smooth muscle cells and thus act vasodilatorily, it cannot be excluded, that progestogens with high affinity to the aldosterone receptor and antimineralocorticoid properties, may exert a strong vasoconstrictory effect. If vascular lesions are present, predominance of the vasoconstrictory action of progestogens may cause acute ischaemic attacks. Therefore, the lowest effective dose of the progestogen has to be used for replacement therapy, and in hysterectomized women, the additional administration of progestogens should be avoided. Similarly, not only the dose of ethinylestradiol, but also that of the respective progestogen in oral contraceptives should be reduced as far as possible. The use of progestogen-dominant ovulation inhibitors should be restricted to cases with an additional indication.