International Journal of Cardiovascular Sciences. 21/May/2020;33(3):215-6.

Oral Contraceptives and Cardiovascular Risk: Adding Clinical Evidence to the Pathophysiology

Daniel Arthur B Kasal ORCID logo , Andrea De Lorenzo ORCID logo

DOI: 10.36660/ijcs.20200078

This Editorial is referred by the Research article "Plasma Renin in Women Using and not Using Combined Oral Contraceptive".

Women cardiovascular health is an important and often neglected issue. Cardiovascular diseases (CVDs) are the main cause of death in women, in Brazil and worldwide. Oral contraceptives are the main method used for contraception in Brazil. The issue of oral contraceptives and cardiovascular risk has been raised since the first descriptions of this class of pharmaceuticals, in the 1960s. The development of low-dose combined oral contraceptives (COCs) containing ethinyl estradiol and different progestins has reduced, albeit not eliminated, cardiovascular morbidity in women taking these medications. The main side effects associated with COCs are procoagulant effects. Therefore, the use of COCs is associated with increased risk of developing acute myocardial infarction, venous thromboembolism and stroke. In addition, adverse changes in the lipid profile and glucose tolerance have been described. Clearly, ageing and exposure to other risk factors, mainly smoking and obesity, play an important role in the development of adverse outcomes related to COCs. In addition, formulations with different progestins may produce distinct effects on circulation.

Another important side effect associated with COCs is the development of hypertension. A meta-analysis including 24 studies and over 250,000 participants found a significant association between the duration of oral contraceptive use and risk of hypertension. Studies regarding the pathophysiology of this association have revealed a number of different and complementary mechanisms. These include oxidative stress, endothelial dysfunction and the activation of the Renin-Angiotensin-Aldosterone system (RAAS). In this issue, Oliveira et al., published an interesting clinical observational study, with young volunteers using low-dose COCs for at least one year, compared to women not using the medication. The authors found higher plasma renin levels in women using COC, with a strong correlation with plasma C-reactive protein (CRP). Additionally, although they did not reach the level of hypertension, systolic arterial pressure measurements of COC users were higher than those of non-users. This finding suggests that RAAS activation, if sustained, could eventually shift blood pressure in women using this medication into the hypertension range. The increase of inflammatory pathways, which is associated with RAAS activation, is also shown by the positive correlation with CRP. While the study was restricted to young and healthy participants, and COC use included five different formulations, the results add clinical evidence linking RAAS activation to oral contraceptive use, inflammation and even hypertension development, in a Brazilian sample.

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Oral Contraceptives and Cardiovascular Risk: Adding Clinical Evidence to the Pathophysiology

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