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Serum metabolome and gut microbiome alterations are associated with low handgrip strength in older adults

机译:血清代谢组和肠道微生物组的改变与老年人握力低有关

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摘要

Handgrip strength (HGS), which represents global muscle strength, is a powerful indicator of disability and mortality in older adults; it is also used for the diagnosis of possible- or probable- sarcopenia and physical frailty. This study aimed to explore the metabolic mechanisms and potential biomarkers associated with declining HGS among older adults. We recruited 15 age- and environment-matched inpatients (age, 77–90 years) with low or normal HGS. Liquid chromatography-mass spectrometry (LC-MS) and 16S ribosomal DNA (rDNA) gene sequencing were performed to analyze the metabolome of serum and stool samples and the gut microbiome composition of stool samples. Spearman’s correlation analysis was used to identify the potential serum and fecal metabolites associated with HGS. We assessed the levels of serum and fecal metabolites belonging to the class of cinnamic acids and derivatives and reported that the levels of carboxylic acids and their derivatives decreased in the low-HGS group. Serum levels of microbial metabolites, including cinnamoylglycine, 4-methoxycinnamic acid, and (e)-3,4,5-trimethoxycinnamic acid, were positively correlated with HGS. We found that gut microbial α-diversity was significantly higher in the low-HGS group, whereas higher β-diversity was observed in the normal group. The relative abundances of the genera Parabacteroides and Intestinibacter increased significantly in the low-HGS group and were negatively correlated with the serum levels of cinnamoylglycine. The identified metabolites whose levels were markedly altered, and intestinal flora associated with these metabolites suggest the potential metabolic underpinnings for HGS and provide a basis for the further identification of biomarkers of muscle strength decline in older adults.
机译:握力 (HGS) 代表整体肌肉力量,是老年人残疾和死亡率的有力指标;它还用于诊断可能或可能的肌肉减少症和身体虚弱。本研究旨在探讨与老年人 HGS 下降相关的代谢机制和潜在生物标志物。我们招募了 15 名年龄和环境匹配的 HGS 低或正常的住院患者 (年龄,77-90 岁)。采用液相色谱-质谱 (LC-MS) 和 16S 核糖体 DNA (rDNA) 基因测序分析血清和粪便样本的代谢组和粪便样本的肠道微生物组组成。采用 Spearman 相关性分析确定与 HGS 相关的潜在血清和粪便代谢物。我们评估了属于肉桂酸及其衍生物类的血清和粪便代谢物的水平,并报告低 HGS 组的羧酸及其衍生物水平降低。血清微生物代谢物(包括肉桂酰甘氨酸、4-甲氧基肉桂酸和 (e)-3,4,5-三甲氧基肉桂酸)水平与 HGS 呈正相关。我们发现低 HGS 组的肠道微生物α多样性显著升高,而正常组观察到较高的β多样性。低 HGS 组副拟杆菌属和肠杆菌属的相对丰度显著增加,与血清肉桂酰甘氨酸水平呈负相关。已鉴定的水平显着改变的代谢物以及与这些代谢物相关的肠道菌群表明 HGS 的潜在代谢基础,并为进一步鉴定老年人肌肉力量下降的生物标志物提供了基础。

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