Urinary Proteomics and Systems Biology Link Eight Proteins to the Higher Risk of Hypertension and Related Complications in Blacks Versus Whites.

IF 3.4 4区生物学 Q2 BIOCHEMICAL RESEARCH METHODS Proteomics Pub Date : 2024-11-24 DOI:10.1002/pmic.202400207

De-Wei An, Dries S Martens, Gontse G Mokwatsi, Yu-Ling Yu, Babangida S Chori, Agnieszka Latosinska, Godsent Isiguzo, Susanne Eder, Dong-Yan Zhang, Gert Mayer, Ruan Kruger, Jana Brguljan-Hitij, Christian Delles, Catharina M C Mels, Katarzyna Stolarz-Skrzypek, Marek Rajzer, Peter Verhamme, Aletta E Schutte, Tim S Nawrot, Yan Li, Harald Mischak, Augustine N Odili, Jan A Staessen

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Abstract

Blacks are more prone to salt-sensitive hypertension than Whites. This cross-sectional analysis of a multi-ethnic cohort aimed to search for proteins potentially involved in the susceptibility to salt sensitivity, hypertension, and hypertension-related complications. The study included individuals enrolled in African Prospective Study on the Early Detection and Identification of Cardiovascular Disease and Hypertension (African-PREDICT), Flemish Study of the Environment, Genes and Health Outcomes (FLEMENGHO), Prospective Cohort Study in Patients with Type 2 Diabetes Mellitus for Validation of Biomarkers (PROVALID)-Austria, and Urinary Proteomics Combined with Home Blood Pressure Telemonitoring for Health Care Reform Trial (UPRIGHT-HTM). Sequenced urinary peptides detectable in 70% of participants allowed the identification of parental proteins and were compared between Blacks and Whites. Of 513 urinary peptides, 300 had significantly different levels among healthy Black (n = 476) and White (n = 483) South Africans sharing the same environment. Analyses contrasting 582 Blacks versus 1731 Whites, and Sub-Saharan Blacks versus European Whites replicated the findings. COL4A1, COL4A2, FGA, PROC, MGP, MYOCD, FYXD2, and UMOD were identified as the most likely candidates underlying the racially different susceptibility to salt sensitivity, hypertension, and related complications. Enriched pathways included hemostasis, platelet activity, collagens, biology of the extracellular matrix, and protein digestion and absorption. Our study suggests that MGP and MYOCD being involved in cardiovascular function, FGA and PROC in coagulation, FYXD2 and UMOD in salt homeostasis, and COL4A1 and COL4A2 as major components of the glomerular basement membrane are among the many proteins potentially incriminated in the higher susceptibility of Blacks compared to Whites to salt sensitivity, hypertension, and its complication. Nevertheless, these eight proteins and their associated pathways deserve further exploration in molecular and human studies as potential targets for intervention to reduce the excess risk of hypertension and cardiovascular complications in Blacks versus Whites.

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尿液蛋白质组学和系统生物学将八种蛋白质与黑人和白人罹患高血压及相关并发症的更高风险联系起来。

黑人比白人更容易患盐敏感性高血压。这项对多种族队列的横断面分析旨在寻找可能与盐敏感性、高血压和高血压相关并发症的易感性有关的蛋白质。研究对象包括参加非洲心血管疾病和高血压早期检测和识别前瞻性研究（African-PREDICT）、弗拉芒环境、基因和健康结果研究（FLEMENGHO）、2型糖尿病患者生物标志物验证前瞻性队列研究（PROVALID）-奥地利、尿液蛋白质组学与家庭血压远程监测相结合促进医疗改革试验（UPRIGHT-HTM）的个人。在 70% 的参与者中检测到的测序尿肽可以确定亲代蛋白，并对黑人和白人进行比较。在 513 种尿液肽中，有 300 种在同一环境下的健康南非黑人（476 人）和白人（483 人）中含量有显著差异。对 582 名黑人与 1731 名白人以及撒哈拉以南黑人与欧洲白人进行的对比分析也证实了这一研究结果。COL4A1、COL4A2、FGA、PROC、MGP、MYOCD、FYXD2 和 UMOD 被确定为盐敏感性、高血压和相关并发症的种族易感性差异的最可能候选基因。丰富的途径包括止血、血小板活性、胶原、细胞外基质生物学以及蛋白质消化和吸收。我们的研究表明，MGP 和 MYOCD 与心血管功能有关，FGA 和 PROC 与凝血有关，FYXD2 和 UMOD 与盐稳态有关，COL4A1 和 COL4A2 是肾小球基底膜的主要成分，这些蛋白质是导致黑人比白人更易患盐敏感、高血压及其并发症的潜在原因。尽管如此，这八种蛋白质及其相关途径仍值得在分子和人体研究中进一步探索，以作为潜在的干预目标，降低黑人相对于白人患高血压和心血管并发症的过高风险。

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来源期刊

Proteomics 生物-生化研究方法

CiteScore

6.30

自引率

5.90%

发文量

193

审稿时长

3 months

期刊介绍： PROTEOMICS is the premier international source for information on all aspects of applications and technologies, including software, in proteomics and other "omics". The journal includes but is not limited to proteomics, genomics, transcriptomics, metabolomics and lipidomics, and systems biology approaches. Papers describing novel applications of proteomics and integration of multi-omics data and approaches are especially welcome.