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人类血小板中低丰度信号蛋白组一个子集的性别依赖性

Gender dependence for a subset of the low-abundance signaling proteome in human platelets.

作者信息

Eidelman Ofer, Jozwik Catherine, Huang Wei, Srivastava Meera, Rothwell Stephen W, Jacobowitz David M, Ji Xiaoduo, Zhang Xiuying, Guggino William, Wright Jerry, Kiefer Jeffrey, Olsen Cara, Adimi Nima, Mueller Gregory P, Pollard Harvey B

机构信息

Department of Anatomy, Physiology and Genetics, USU Center for Medical Proteomics, Uniformed Services University, School of Medicine, USUHS, 4301 Jones Bridge Road, Bethesda, MD 20814, USA.

出版信息

Hum Genomics Proteomics. 2010 Apr 13;2010:164906. doi: 10.4061/2010/164906.

Abstract

The incidence of cardiovascular diseases is ten-times higher in males than females, although the biological basis for this gender disparity is not known. However, based on the fact that antiplatelet drugs are the mainstay for prevention and therapy, we hypothesized that the signaling proteomes in platelets from normal male donors might be more activated than platelets from normal female donors. We report here that platelets from male donors express significantly higher levels of signaling cascade proteins than platelets from female donors. In silico connectivity analysis shows that the 24 major hubs in platelets from male donors focus on pathways associated with megakaryocytic expansion and platelet activation. By contrast, the 11 major hubs in platelets from female donors were found to be either negative or neutral for platelet-relevant processes. The difference may suggest a biological mechanism for gender discrimination in cardiovascular disease.

摘要

心血管疾病的发病率男性比女性高十倍,尽管这种性别差异的生物学基础尚不清楚。然而,基于抗血小板药物是预防和治疗的主要手段这一事实,我们推测正常男性供体血小板中的信号蛋白质组可能比正常女性供体血小板中的更活跃。我们在此报告,男性供体的血小板比女性供体的血小板表达显著更高水平的信号级联蛋白。计算机连接性分析表明,男性供体血小板中的24个主要枢纽集中在与巨核细胞扩增和血小板活化相关的途径上。相比之下,女性供体血小板中的11个主要枢纽在与血小板相关的过程中被发现是负性或中性的。这种差异可能提示了心血管疾病中性别差异的生物学机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4a19/2958630/7d0bf5c72dac/HGP2010-164906.001.jpg

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