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与 HIV 共存的老年人中,与年龄相关的肠道菌群失调,表现为丁酸盐生成潜能丧失,与血浆色氨酸代谢物改变相关。

Age-Associated Gut Dysbiosis, Marked by Loss of Butyrogenic Potential, Correlates With Altered Plasma Tryptophan Metabolites in Older People Living With HIV.

机构信息

Department of Medicine, University of Louisville, KY.

Alcohol Research Center, University of Louisville, KY.

出版信息

J Acquir Immune Defic Syndr. 2022 Feb 1;89(Suppl 1):S56-S64. doi: 10.1097/QAI.0000000000002866.

Abstract

BACKGROUND

Imbalance in tryptophan (TRP) metabolism and its neuroactive metabolites, serotonin and kynurenine (KYN), is a known pathogenic mechanism underlying neurocognitive impairment. Gut microbiota plays an important role in TRP metabolism, and the production of these neuroactive molecules affects neurocognitive function. Although both HIV infection and normal aging independently induce gut dysbiosis and influence TRP metabolism, their interactive effects on compositional/functional changes in gut microbiota and consequent alterations in TRP metabolites remain largely undetermined.

METHODS

Older people living with HIV infection (PLWH, aged 50-70 years, n = 22) were enrolled in this cross-sectional pilot study. Metagenomic analysis of fecal microbiome using 16S Ribosomal ribonucleic acid gene sequencing and metabolomics analysis of plasma using mass spectrometry with a reverse-phase iquid chromatography tandem mass spectrometry were performed. Statistical analyses included the univariate linear regression and Spearman correlation analyses.

RESULTS

Age-associated changes in plasma levels of key neuroactive TRP metabolites, serotonin and KYN, were seen in PLWH. Specifically, we observed age-dependent decreases in serotonin and increases in KYN and KYN-to-TRP ratio, indicative of dysfunctional TRP metabolism. Furthermore, the gut dysbiosis seen in older PLWH is characterized by a reduction of Firmicutes/Bacteroidetes ratio and butyrate-producing microbial families Lachnospiraceae and Lactobacillaceae. Of importance, correspondent with gut dysbiosis, increasing age was significantly associated with decreased plasma butyrate levels, which in turn correlated positively with serotonin and negatively with KYN/TRP ratio.

CONCLUSIONS

Age-dependent gut microbial dysbiosis distinguished by a decrease in butyrogenic potential is a key pathogenic feature associated with the shift in TRP metabolism from serotonin to KYN in older PLWH.

摘要

背景

色氨酸(TRP)代谢及其神经活性代谢物 5-羟色胺(serotonin)和犬尿氨酸(kynurenine,KYN)的失衡是导致神经认知功能障碍的已知发病机制。肠道微生物群在 TRP 代谢中起着重要作用,这些神经活性分子的产生会影响神经认知功能。虽然 HIV 感染和正常衰老都会独立引起肠道菌群失调并影响 TRP 代谢,但它们对肠道微生物群组成/功能变化的相互作用以及由此导致的 TRP 代谢物的改变仍很大程度上尚未确定。

方法

本横断面研究纳入了年龄在 50-70 岁的 HIV 感染者(PLWH,n=22)。采用 16S 核糖体 RNA 基因测序进行粪便微生物组的宏基因组分析,采用反相液相色谱串联质谱法进行血浆代谢组学分析。统计分析包括单变量线性回归和 Spearman 相关分析。

结果

PLWH 中观察到与年龄相关的血浆中关键神经活性 TRP 代谢物 5-羟色胺和 KYN 水平的变化。具体来说,我们观察到 5-羟色胺随年龄的依赖性降低,KYN 和 KYN-TRP 比值增加,提示 TRP 代谢功能障碍。此外,在年龄较大的 PLWH 中观察到的肠道菌群失调表现为厚壁菌门/拟杆菌门比值降低,以及丁酸产生菌科 Lachnospiraceae 和乳杆菌科减少。重要的是,与肠道菌群失调相一致的是,随着年龄的增长,血浆丁酸水平显著降低,而丁酸水平与 5-羟色胺呈正相关,与 KYN/TRP 比值呈负相关。

结论

依赖年龄的肠道微生物失调,其特征是丁酸生成潜力下降,是与年龄较大的 PLWH 中 TRP 代谢从 5-羟色胺向 KYN 转移相关的关键发病特征。

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