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心脏应激中的性别和性激素——机制见解。

Sex and sex hormones in cardiac stress--mechanistic insights.

机构信息

Department of Physiology, University of Melbourne, Victoria, Australia.

出版信息

J Steroid Biochem Mol Biol. 2013 Sep;137:124-35. doi: 10.1016/j.jsbmb.2013.05.015. Epub 2013 Jun 13.

DOI:10.1016/j.jsbmb.2013.05.015
PMID:23770428
Abstract

Important sex differences in the onset and characteristics of cardiovascular disease are evident, yet the mechanistic details remain unresolved. Men are more susceptible to cardiovascular disease earlier in life, though younger women who have a cardiovascular event are more likely to experience adverse outcomes. Emerging evidence is prompting a re-examination of the conventional view that estrogen is protective and testosterone a liability. The heart expresses both androgen and estrogen receptors and is functionally responsive to circulating sex steroids. New evidence of cardiac aromatase expression indicates local estrogen production may also exert autocrine/paracrine actions in the heart. Cardiomyocyte contractility studies suggest testosterone and estrogen have contrasting inotropic actions, and modulate Ca(2+) handling and transient characteristics. Experimentally, sex differences are also evident in cardiac stress responses. Female hearts are generally less susceptible to acute ischemic damage and associated arrhythmias, and generally are more resistant to stress-induced hypertrophy and heart failure, attributed to the cardioprotective actions of estrogen. However, more recent data show that testosterone can also improve acute post-ischemic outcomes and facilitate myocardial function and survival in chronic post-infarction. The myocardial actions of sex steroids are complex and context dependent. A greater mechanistic understanding of the specific actions of systemic/local sex steroids in different cardiovascular disease states has potential to lead to the development of cardiac therapies targeted specifically for men and women.

摘要

重要的性别差异在发病和心血管疾病的特点是显而易见的,但机械学细节仍未解决。男性更容易患心血管疾病,在生命的早期,尽管年轻的妇女有心血管事件更可能经历不良后果。新兴的证据促使重新审查传统的观点,即雌激素是保护,睾丸激素是责任。心脏表达雄激素和雌激素受体,并对循环性激素的功能反应。心脏芳香化酶表达的新证据表明,局部雌激素的产生也可能发挥自分泌/旁分泌作用在心脏。心肌收缩性研究表明,睾丸激素和雌激素具有相反的变力作用,并调节 Ca(2+)处理和瞬态特征。实验中,性别差异也明显在心脏应激反应。女性心脏一般不太容易受到急性缺血性损伤和相关的心律失常,一般更耐受应激诱导的肥大和心力衰竭,归因于雌激素的心脏保护作用。然而,最近的数据表明,睾丸激素也可以改善急性缺血后结果,并促进慢性心肌梗死后心肌功能和存活。性类固醇的心肌作用是复杂的和上下文相关的。对系统性/局部性激素在不同心血管疾病状态下的具体作用有更深入的了解,有可能导致开发出专门针对男性和女性的心脏治疗方法。

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