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四肢骨骼肌质量和握力的靶向蛋白质组学在南非黑人中的横断面研究。

Targeted proteomics of appendicular skeletal muscle mass and handgrip strength in black South Africans: a cross-sectional study.

机构信息

SAMRC/Wits Developmental Pathways for Health Research Unit, School of Clinical Medicine, Faculty of Health Sciences, University of the Witwatersrand, Johannesburg, South Africa.

Global Health Research Institute, School of Health and Human Development, University of Southampton, Southampton, UK.

出版信息

Sci Rep. 2022 Jun 9;12(1):9512. doi: 10.1038/s41598-022-13548-9.

Abstract

Although appendicular skeletal muscle mass (ASM) and handgrip strength (HGS) are key components of sarcopenia, their underlying biological mechanisms remain poorly understood. We aimed to investigate associations of circulating biomarkers with ASM and HGS in middle-aged black South Africans. This study consisted of 934 black South Africans (469 men and 465 women, aged 41-72 years) from the Middle-aged Soweto cohort. Linear regression models were used to examine relationships between 182 biomarkers (measured with proximity extension assay) and dual-energy X-ray absorptiometry-measured ASM and dynamometer-measured HGS. Age, height, sex, smoking, alcohol, food insecurity, physical activity, visceral adipose tissue, HIV and menopausal status were included as confounders. Regression models showing sex-interactions were stratified by sex. The Benjamini-Hochberg false discovery rate (FDR) was used to control for multiple testing, and FDR-adjusted P values were reported. In the total sample, 10 biomarkers were associated with higher ASM and 29 with lower ASM (P < 0.05). Out of these 39 biomarkers, 8 were also associated with lower HGS (P < 0.05). MMP-7 was associated with lower HGS only (P = 0.011) in the total sample. Sex-interactions (P < 0.05) were identified for 52 biomarkers for ASM, and 6 for HGS. For men, LEP, MEPE and SCF were associated with higher ASM (P < 0.001, = 0.004, = 0.006, respectively), and MEPE and SCF were also associated with higher HGS (P = 0.001, 0.012, respectively). Also in men, 37 biomarkers were associated with lower ASM (P < 0.05), with none of these being associated with lower HGS. Furthermore, DLK-1 and MYOGLOBIN were associated with higher HGS only (P = 0.004, 0.006, respectively), while GAL-9 was associated with lower HGS only (P = 0.005), among men. For women, LEP, CD163, IL6, TNF-R1 and TNF-R2 were associated with higher ASM (P < 0.001, = 0.014, = 0.027, = 0.014, = 0.048, respectively), while IGFBP-2, CTRC and RAGE were associated with lower ASM (P = 0.043, 0.001, 0.014, respectively). No biomarker was associated with HGS in women. In conclusion, most biomarkers were associated with ASM and not HGS, and the associations of biomarkers with ASM and HGS displayed sex-specificity in middle-aged black South Africans. Proteomic studies should examine ASM and HGS individually. Future research should also consider sexual dimorphism in the pathophysiology of sarcopenia for development of sex-specific treatment and diagnostic methods.

摘要

虽然附肢骨骼肌质量(ASM)和握力(HGS)是肌少症的关键组成部分,但它们的潜在生物学机制仍知之甚少。我们旨在研究循环生物标志物与中年南非黑人的 ASM 和 HGS 之间的关联。本研究包括来自南非索韦托中年队列的 934 名南非黑人(469 名男性和 465 名女性,年龄 41-72 岁)。使用线性回归模型来检查 182 种生物标志物(使用接近延伸测定法测量)与双能 X 射线吸收仪测量的 ASM 和测力计测量的 HGS 之间的关系。年龄、身高、性别、吸烟、饮酒、食物不安全、身体活动、内脏脂肪组织、HIV 和绝经状态被纳入混杂因素。显示性别相互作用的回归模型按性别分层。使用 Benjamini-Hochberg 假发现率(FDR)控制多重检验,并报告 FDR 调整后的 P 值。在总样本中,有 10 种生物标志物与较高的 ASM 相关,29 种与较低的 ASM 相关(P < 0.05)。在这 39 种生物标志物中,有 8 种还与较低的 HGS 相关(P < 0.05)。在总样本中,MMP-7 仅与较低的 HGS 相关(P = 0.011)。性别相互作用(P < 0.05)在 52 种 ASM 生物标志物和 6 种 HGS 生物标志物中被确定。对于男性,LEP、MEPE 和 SCF 与较高的 ASM 相关(P < 0.001、= 0.004、= 0.006,分别),MEPE 和 SCF 也与较高的 HGS 相关(P = 0.001、0.012,分别)。同样在男性中,有 37 种生物标志物与较低的 ASM 相关(P < 0.05),但没有一种与较低的 HGS 相关。此外,DLK-1 和 MYOGLOBIN 仅与较高的 HGS 相关(P = 0.004、0.006,分别),而 GAL-9 仅与较低的 HGS 相关(P = 0.005)。对于女性,LEP、CD163、IL6、TNF-R1 和 TNF-R2 与较高的 ASM 相关(P < 0.001、= 0.014、= 0.027、= 0.014、= 0.048,分别),而 IGFBP-2、CTRC 和 RAGE 与较低的 ASM 相关(P = 0.043、0.001、0.014,分别)。没有生物标志物与女性的 HGS 相关。总之,大多数生物标志物与 ASM 相关,而与 HGS 无关,并且生物标志物与 ASM 和 HGS 的关联在南非中年黑人中表现出性别特异性。蛋白质组学研究应单独检查 ASM 和 HGS。未来的研究还应考虑肌少症病理生理学中的性别二态性,以开发针对男性和女性的特定治疗和诊断方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/44ac/9184732/3734b2a116c8/41598_2022_13548_Fig1_HTML.jpg

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