Sexual Dimorphism of Plasma and Tissue Proteomes in Human Calcific Aortic Valve Stenosis Pathogenesis-Brief Report.

IF 7.4 1区医学 Q1 HEMATOLOGY

Arteriosclerosis, Thrombosis, and Vascular Biology Pub Date : 2025-10-01 Epub Date: 2025-08-14 DOI:10.1161/ATVBAHA.125.322560

Cassandra L Clift, Mark C Blaser, Francesca Bartoli-Leonard, Florian Schlotter, Hideyuki Higashi, Shiori Kuraoka, Taku Kasai, Mandy E Turner, Tan Pham, Katelyn A Perez, Simon C Robson, Simon C Body, Jochen D Muehlschlegel, Masanori Aikawa, Sasha A Singh, Elena Aikawa

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引用次数: 0

Abstract

Background: Calcific aortic valve stenosis is a global clinical burden, impacting around 2% of the population over 65 years of age. No pharmacotherapeutics exist, with surgical repair and transcatheter valve replacement being the only intervention. Females are underrepresented in studies of calcific aortic valve stenosis, leading to delay in timely intervention and increased mortality. Histopathology demonstrates female calcific aortic valve stenosis presents with decreased valvular calcification but increased fibrosis and severity of symptoms. We hypothesize that the underlying molecular mechanisms contributing to disease progression and fibrocalcific burden in aortic stenosis (AS) differ between male and female patients. Our goal for this study is to use previously acquired proteomic data sets of a clinically defined human AS cohort to examine sex disparities and underlying sex-specific disease signatures.

Methods: Age-matched human AS tissue samples (n=14 males, n=4 females) were each segmented into nondiseased, fibrotic, and calcified disease stages and analyzed using LC-MS/MS (liquid chromatrophy tandem mass spectrometry) proteomics and quantitative histopathology. AS plasma samples (n=32 males, n=20 females) were analyzed for circulating sex-specific biomarkers via LC-MS/MS.

Results: Unbiased principal component analysis shows sex- and stage-specific proteome clustering. AS pathogenesis drove sex-specific disparities in the valvular proteome: 338/1503 total proteins were differentially enriched by sex across disease stages. Compared with sex-specific nondiseased controls, female fibrotic tissue resulted in 2.75-fold greater number of differentially enriched proteins than did male fibrotic tissue (female: 42, male: 16; P<0.05 threshold). In contrast, female calcific tissue identified 2.473-fold less differentially enriched proteins than male calcific tissue (female: 157, male 356; P<0.05 threshold). Functional Enrichment Analysis revealed specific proteins responsible for the exacerbated valvular fibrosis signature in females, implicated adenosine phosphate metabolism as a potential male-specific driver of AS, and further reinforced the shared contribution of aberrant lipid and cholesterol activity to AS progression in both sexes.

Conclusions: This proof-of-concept analysis allows for the identification of potential sex-specific protein drug targets implicated in AS pathobiology.

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人钙化主动脉瓣狭窄发病过程中血浆和组织蛋白质组的性别二态性。

背景：钙化性主动脉瓣狭窄是一种全球性的临床负担，影响约2%的65岁以上人群。没有药物治疗存在，手术修复和经导管瓣膜置换术是唯一的干预措施。女性在钙化主动脉瓣狭窄的研究中代表性不足，导致及时干预的延迟和死亡率的增加。组织病理学显示女性钙化性主动脉瓣狭窄表现为瓣膜钙化减少，但纤维化增加和症状严重。我们假设导致主动脉瓣狭窄（AS）疾病进展和纤维钙化负担的潜在分子机制在男性和女性患者之间存在差异。我们这项研究的目标是使用先前获得的临床定义的人类AS队列的蛋白质组学数据集来检查性别差异和潜在的性别特异性疾病特征。方法：将年龄匹配的人类AS组织样本（男性14例，女性4例）分别分为非病变、纤维化和钙化病变阶段，并使用LC-MS/ms蛋白质组学和定量组织病理学进行分析。通过LC-MS/ms分析AS血浆样本（n=32男性，n=20女性）的循环性别特异性生物标志物。结果：无偏主成分分析显示性别和阶段特异性蛋白质组聚类。AS发病机制驱动瓣膜蛋白组的性别特异性差异：在疾病阶段，338/1503总蛋白的富集程度因性别而异。与性别特异性的未患病对照组相比，女性纤维化组织产生的差异富集蛋白数量是男性纤维化组织的2.75倍(女性：42，男性：16；pq结论：这种概念验证分析允许鉴定与AS病理生物学相关的潜在性别特异性蛋白质药物靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Arteriosclerosis, Thrombosis, and Vascular Biology 医学-外周血管病

CiteScore

15.60

自引率

2.30%

发文量

337

审稿时长

2-4 weeks

期刊介绍： The journal "Arteriosclerosis, Thrombosis, and Vascular Biology" (ATVB) is a scientific publication that focuses on the fields of vascular biology, atherosclerosis, and thrombosis. It is a peer-reviewed journal that publishes original research articles, reviews, and other scholarly content related to these areas. The journal is published by the American Heart Association (AHA) and the American Stroke Association (ASA). The journal was published bi-monthly until January 1992, after which it transitioned to a monthly publication schedule. The journal is aimed at a professional audience, including academic cardiologists, vascular biologists, physiologists, pharmacologists and hematologists.