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血浆 C 端神经黏附蛋白片段作为肌少症的早期生物标志物:GenoFit 研究结果。

Plasma C-Terminal Agrin Fragment as an Early Biomarker for Sarcopenia: Results From the GenoFit Study.

机构信息

Institute for Sport and Health, University College Dublin, Ireland.

Genuity Science, Dublin, Ireland.

出版信息

J Gerontol A Biol Sci Med Sci. 2021 Nov 15;76(12):2090-2096. doi: 10.1093/gerona/glab139.

Abstract

Barriers associated with direct muscle quantification have prevented a consistent implementation of therapeutic measures for sarcopenia. Recently, the relevance of circulating C-terminal agrin fragment (CAF) as an accessible screening method alternative for sarcopenia has gained credence. Accordingly, this study aimed to verify the pertinence of plasma CAF as a biomarker for sarcopenia. Three hundred healthy adults aged between 50 and 83 years took part in this study. Sarcopenia was diagnosed according to the European Working Group on Sarcopenia in Older People criteria. Body composition was assessed using dual-energy x-ray absorptiometry, while muscle strength was examined using hand dynamometry. Plasma CAF concentrations were determined using a commercially available ELISA kit. CAF concentrations were significantly associated with appendicular lean mass (ALM), but not grip strength (p = .028, p = .575, respectively). Plasma CAF concentrations were significantly elevated in sarcopenic individuals compared to nonsarcopenic (p < .001). Overall, individuals with low grip strength or low ALM displayed significantly higher CAF levels compared to healthy controls, after adjusting for age and body mass index (p = .027, p = .003, respectively). In males, those with low grip strength or low ALM had significantly elevated CAF levels (p = .039, p = .027, respectively), while in females, only those with low ALM had significantly raised CAF concentrations, compared to healthy controls (p = .035). Our findings illuminate the potential relevance of CAF as an accessible biomarker for skeletal muscle health. CAF determination may enhance clinical practice by facilitating more widespread treatment strategies for sarcopenia. Nevertheless, future research is needed to confirm the diagnostic pertinence of CAF concentrations in screening for sarcopenia.

摘要

与直接肌肉定量相关的障碍阻碍了对肌少症的治疗措施的一致实施。最近,循环 C 端聚集素片段(CAF)作为肌少症的一种可行的筛选方法替代物的相关性得到了认可。因此,本研究旨在验证血浆 CAF 作为肌少症生物标志物的相关性。300 名年龄在 50 至 83 岁之间的健康成年人参与了这项研究。肌少症根据欧洲老年人肌少症工作组的标准进行诊断。使用双能 X 射线吸收法评估身体成分,使用握力计评估肌肉力量。使用商业上可获得的 ELISA 试剂盒测定血浆 CAF 浓度。CAF 浓度与四肢瘦质量(ALM)显著相关,但与握力无关(p =.028,p =.575)。与非肌少症个体相比,肌少症个体的血浆 CAF 浓度显著升高(p <.001)。总体而言,与健康对照组相比,握力或 ALM 低的个体的 CAF 水平显著升高,调整年龄和体重指数后(p =.027,p =.003)。在男性中,握力或 ALM 低的个体的 CAF 水平显著升高(p =.039,p =.027),而在女性中,仅 ALM 低的个体的 CAF 浓度显著升高,与健康对照组相比(p =.035)。我们的发现阐明了 CAF 作为骨骼肌肉健康的一种可行生物标志物的潜在相关性。CAF 测定可能通过促进更广泛的肌少症治疗策略来增强临床实践。然而,需要进一步的研究来确认 CAF 浓度在肌少症筛查中的诊断相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7bbd/8599080/e7fa40619ebe/glab139f0001.jpg

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