Fecal Microbiota and Associated Metabolites Are Minimally Affected by Ten Weeks of Resistance Training in Younger and Older Adults.

IF 2.2 Q2 SPORT SCIENCES

Sports Pub Date : 2025-03-26 DOI:10.3390/sports13040098

Anthony Agyin-Birikorang, Sarah Lennon, Kristen S Smith, William Van Der Pol, Morgan A Smith, Casey L Sexton, Donald A Lamb, Kaelin C Young, Christopher Brooks Mobley, Kevin W Huggins, Michael D Roberts, Andrew Dandridge Frugé

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Abstract

Preclinical evidence suggests that short chain fatty acids (SCFAs) produced by gut microbiota may impact body composition and muscle growth. While aging is implicated in negative alterations to the gut microbiome, exercise may mitigate these changes. Limited human evidence indicates that resistance training (RT) does not appreciably alter the gut microbiome in older adults, and no human study has examined whether resistance training differentially alters the gut microbiome and associated SCFAs between younger and older individuals. Therefore, we examined whether 10 weeks of RT differentially altered fecal microbiota composition, fecal and circulating SCFAs, and serum markers associated with gastrointestinal integrity in two cohorts of adults. Fecal and serum samples were obtained from untrained younger (22 ± 2 years, n = 12) and older (58 ± 8 years, n = 12) participants prior to and following 10 weeks of supervised twice-weekly full-body RT. Outcome measures immediately before (PRE) and after the intervention (POST) included dual X-ray absorptiometry for body composition, ultrasound for vastus lateralis (VL) thickness, 16S rRNA gene sequencing fecal microbiome data, serum and fecal SCFAs measured by gas chromatography, and serum intestinal fatty acid-binding protein 2 (FABP2), lipopolysaccharide-binding protein (LBP), and leucine-rich alpha-2 glycoprotein (LRG-1) quantified by enzyme-linked immunosorbent assays. Main effects and interactions were measured by repeated measures analysis of variance (group × time; G × T) for all dependent variables, and Spearman correlations were used to explore relationships among changes in relevant outcomes. The intervention significantly increased VL thickness and lean body mass (p < 0.05) equally in both groups. Although group differences in microbiome beta diversity were identified, no effects of age, time, or their interaction were observed for the alpha diversity measures. Seven SCFAs were detected in the fecal samples, albeit no significant age, time, or interaction effects were evident. In serum, acetic acid was the only SCFA detected, with no significant age, time, or interaction effects. Serum LRG1 decreased for all participants (p = 0.007) with higher levels in younger adults (p = 0.015), but no G × T interactions were observed for this marker, serum FABP2, or LBP. No significant correlations were observed among RT-induced changes in muscle mass-related outcomes and changes in fecal microbiome diversity, total or individual SCFAs, or serum FABP2/LBP/LRG-1. These results highlight that 10 weeks of RT largely does not affect fecal microbiota, associated SCFAs, or select markers of gastrointestinal integrity in untrained younger or older adults.

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在年轻人和老年人中，10周的阻力训练对粪便微生物群和相关代谢物的影响最小。

临床前证据表明，肠道菌群产生的短链脂肪酸（SCFAs）可能影响身体成分和肌肉生长。虽然衰老与肠道微生物群的负面变化有关，但锻炼可能会减轻这些变化。有限的人类证据表明，阻力训练（RT）不会明显改变老年人的肠道微生物群，并且没有人类研究检验阻力训练是否会在年轻人和老年人之间改变肠道微生物群和相关的scfa。因此，我们在两组成年人中研究了10周的RT治疗是否会改变粪便微生物群组成、粪便和循环SCFAs以及与胃肠道完整性相关的血清标志物。从未经训练的年轻（22±2岁，n = 12）和老年（58±8岁，n = 12）参与者中获取粪便和血清样本，在为期10周的监督下每周两次的全身rt之前和之后。干预前（PRE）和干预后（POST）的结果测量包括身体成分的双x线吸收仪、股外侧肌（VL）厚度的超声、16S rRNA基因测序粪便微生物组数据、血清和粪便SCFAs气相色谱测量。酶联免疫吸附法测定血清肠道脂肪酸结合蛋白2 （FABP2）、脂多糖结合蛋白（LBP）和富含亮氨酸的α -2糖蛋白（LRG-1）。主效应和相互作用采用重复测量方差分析(组×时间；G × T)表示所有因变量，并使用Spearman相关来探讨相关结果变化之间的关系。干预组VL厚度和瘦体质量均显著增加（p < 0.05）。虽然确定了微生物组β多样性的组间差异，但没有观察到年龄、时间或它们之间的相互作用对α多样性的影响。在粪便样本中检测到7种SCFAs，尽管没有明显的年龄、时间或相互作用效应。在血清中，醋酸是唯一检测到的SCFA，没有明显的年龄、时间或相互作用影响。所有参与者的血清LRG1均下降（p = 0.007），年轻人的血清LRG1水平较高（p = 0.015），但未观察到该标志物、血清FABP2或LBP之间的G × T相互作用。rt诱导的肌肉质量相关结果的变化与粪便微生物群多样性、总或个体scfa或血清FABP2/LBP/LRG-1的变化之间没有显著相关性。这些结果强调，在未经训练的年轻人或老年人中，10周的RT在很大程度上不会影响粪便微生物群、相关的scfa或胃肠道完整性的选择标志物。

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