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The influence of biological sex and sex hormones on bile acid synthesis and cholesterol homeostasis

机译:生物性交和性激素对胆汁酸合成和胆固醇稳态的影响

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Obesity and elevated serum lipids are associated with a threefold increase in the risk of developing atherosclerosis, a condition that underlies stroke, myocardial infarction, and sudden cardiac death. Strategies that aim to reduce serum cholesterol through modulation of liver enzymes have been successful in decreasing the risk of developing atherosclerosis and reducing mortality. Statins, which inhibit cholesterol biosynthesis in the liver, are considered among the most successful compounds developed for the treatment of cardiovascular disease. However, recent debate surrounding their effectiveness and safety prompts consideration of alternative cholesterol-lowering therapies, including increasing cholesterol catabolism through bile acid (BA) synthesis. Targeting the enzymes that convert cholesterol to BAs represents a promising alternative to other cholesterol-lowering approaches that treat atherosclerosis as well as fatty liver diseases and diabetes mellitus. Compounds that modify the activity of these pathways have been developed; however, there remains a lack of consideration of biological sex. This is necessary in light of strong evidence for sexual dimorphisms not only in the incidence and progression of the diseases they influence but also in the expression and activity of the proteins affected and in the manner in which men and women respond to drugs that modify lipid handling in the liver. A thorough understanding of the enzymes involved in cholesterol catabolism and modulation by biological sex is necessary to maximize their therapeutic potential.
机译:肥胖症和升高的血清脂质与三倍的增加有关的患者粥样硬化的风险,是下潜,心肌梗塞和突然心脏死亡的病症。通过调节肝脏酶来减少血清胆固醇的策略已经成功地降低了发展动脉粥样硬化和降低死亡率的风险。抑制肝脏中胆固醇生物合成的他汀类药物被认为是用于治疗心血管疾病的最成功的化合物。然而,近期争论围绕其有效性和安全促使替代胆固醇降低疗法,包括通过胆汁酸(BA)合成增加胆固醇分解代谢。靶向将胆固醇转化为BAS的酶代表了对治疗动脉粥样硬化以及脂肪肝病和糖尿病的其他胆固醇降低方法的有希望的替代方法。已经开发了改变这些途径的活性的化合物;但是,仍然缺乏对生物性别的思考。这是必要的,即不仅在其影响的疾病的发病率和进展中的性别二态性的强有力证据,而且是影响蛋白质的表达和活性,也是男女和妇女对修改脂质处理的药物的方式在肝脏。彻底了解参与胆固醇分解代谢和通过生物性调节的酶来最大限度地提高其治疗潜力。

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