性激素在腹主动脉瘤中的作用:专题综述。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2023-11-27 Epub Date: 2023-08-17 DOI:10.21037/acs-2023-adw-17
Rebecka Hultgren
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引用次数: 0

摘要

几十年来,腹主动脉瘤(AAA)患者的性别差异一直有报道。男性发病率更高、发病时间更早、阻碍修复的形态特征更少、短期和长期存活率更高。近年来,人们曾多次尝试找出导致这些性别差异的生物或致病因素,包括社会经济因素,但都以失败告终。最大的挑战是揭示男女发病的不同机制,其次是确定导致疾病进展和最终破裂的因素。对已确诊患者进行的评估未能发现任何与疾病发展相关的因素,而这些因素可以明确解释深刻的性别差异。考虑到男性发病的诱因明显早于女性,排除吸烟、高血压、高脂血症等唯一可证明的诱因,剩下需要探讨的因素就是性激素或生物机制。本专题综述探讨了有关性激素及其与女性和男性 AAA 关联的当代出版物。研究结果证实,女性和男性性激素对动脉瘤疾病的发生或发展的影响缺乏科学证据。一些微弱的迹象表明,受吸烟和遗传的影响,女性可能受益于较长的生育史,从而有助于防止动脉瘤的发展。有证据表明,与其他表现形式的心血管疾病一样,男性睾酮水平过低也会增加 AAA 的发病风险。至于女性性激素循环水平较高对男性发病风险的影响,还有待评估。总之,在未来十年中,这一领域将不断扩大,通过结合基于登记和转化的数据库,对女性和男性进行分层分析,为我们提供更多的证据,有助于对未来有发生 AAA 风险的人群进行重要的风险因素评估。
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The role of sex hormones in abdominal aortic aneurysms: a topical review.

Sex discrepancies have been reported for patients with abdominal aortic aneurysm (AAA) for decades. Men have a higher prevalence of disease, earlier onset, less morphological features obstructing eligibility for repair and better survival, both short and long term. In more recent years, several attempts have been made to identify the biologic or pathogenic factors contributing to these sex differences, including socioeconomic factors though all have failed. The greatest challenge is to reveal the variable mechanism for development of disease for both women and men, and secondly to identify the factors contributing to the progression of disease, and eventual rupture. Evaluations of diagnosed patients have failed to detect any factors associated with development of disease which would give a distinct explanation for the profound sex differences. Considering the obvious earlier trigger for development in men compared to women, excluding smoking, hypertension, hyperlipidemia as certified sole triggers, the remaining factors to explore are sex hormones or biological mechanisms. This topical review explores the contemporary publications on sex hormones and their association with AAA in women and men. The findings confirm the lack of scientific evidence for the influence of female and male sex hormones on development or progression of aneurysm disease. Weak indications support that women probably benefit from a longer reproductive history as a contributing protection against AAA development, influenced by smoking and heredity. There is some evidence that could support that, as for other manifestations of cardiovascular diseases, low testosterone levels in men, can contribute to an increased risk for AAA development. The influence of higher circulating levels of female sex hormones on risk development in men remains to be evaluated. In conclusion, this area will expand during the next decade, by combining registry-based and translational databases in stratified analysis for women and men, giving us more evidence that will contribute to important risk factor estimations for future cohorts at risk of AAA development.

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