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肝性脑病患者对利福昔明的反应存在明显差异,这取决于功能性肠道微生物种类。

Distinct responsiveness to rifaximin in patients with hepatic encephalopathy depends on functional gut microbial species.

机构信息

Department of PathophysiologyGraduate School of MedicineOsaka Metropolitan University (formerly, Osaka City University)OsakaJapan.

Department of HepatologyGraduate School of MedicineOsaka Metropolitan University (formerly, Osaka City University)OsakaJapan.

出版信息

Hepatol Commun. 2022 Aug;6(8):2090-2104. doi: 10.1002/hep4.1954. Epub 2022 Apr 16.

Abstract

Hepatic encephalopathy (HE) is the neuropsychiatric complication of liver cirrhosis (LC). The influence of gut microbiota on HE pathogenesis has been suggested but not precisely elucidated. Here, we investigate how the gut microbial profile changed in patients with HE to clarify the functional gut microbial species associated with HE. We focused on their responses to rifaximin (RFX), a nonabsorbable antibiotic used in HE therapy. Feces samples were collected from patients with decompensated LC (all HE), patients with compensated LC, and healthy controls, and fecal gut microbial profiles were compared using 16S ribosomal RNA gene amplicon and metagenomic sequencing. The linear discriminant analysis effect size was used to identify specific species. Urease-positive Streptococcus salivarius, which can produce ammonia, was identified as the most significantly abundant gut microbiota in the HE group, and its ability to elevate the levels of blood ammonia as well as brain glutamine was experimentally verified in mice. Urease-negative Ruminococcus gnavus was also identified as a significantly abundant species in patients with RFX-nonresponsive HE after RFX administration. Interestingly, R. gnavus enhanced urease activity of recombinant urease itself, implying that R. gnavus could amplify ammonia production of surrounding urease-positive microbiota. Furthermore, the sensitivity of S. salivarius and R. gnavus to RFX depended on conjugated secondary bile acid levels, suggesting a therapeutic potential of the combined use of secondary bile acid levels with RFX for enhancing the efficacy of RFX. This study identified specific gut bacterial species abundant in patients with HE and verified their functions linked to HE pathophysiology. Targeting these bacteria could be a potentially effective strategy to treat HE.

摘要

肝性脑病 (HE) 是肝硬化 (LC) 的神经精神并发症。肠道微生物群对 HE 发病机制的影响已被提出,但尚未得到明确阐明。在这里,我们研究了 HE 患者肠道微生物谱的变化,以阐明与 HE 相关的功能性肠道微生物种类。我们专注于它们对利福昔明 (RFX) 的反应,RFX 是一种用于 HE 治疗的不可吸收抗生素。从失代偿性 LC 患者(所有 HE)、代偿性 LC 患者和健康对照中收集粪便样本,并使用 16S 核糖体 RNA 基因扩增子和宏基因组测序比较粪便肠道微生物谱。使用线性判别分析效应大小来识别特定物种。产脲酶的唾液链球菌被鉴定为 HE 组中最显著丰富的肠道微生物群,其在小鼠体内升高血氨和脑谷氨酰胺的能力得到了实验验证。在 RFX 给药后 RFX 无反应性 HE 患者中,也鉴定出产脲酶阴性的罗氏真杆菌是一种显著丰富的物种。有趣的是,R. gnavus 增强了重组脲酶本身的脲酶活性,这表明 R. gnavus 可以放大周围产脲酶阳性微生物的氨产量。此外,S. salivarius 和 R. gnavus 对 RFX 的敏感性取决于结合型次级胆汁酸水平,这表明联合使用次级胆汁酸水平和 RFX 来增强 RFX 的疗效具有治疗潜力。本研究鉴定了 HE 患者中丰富的特定肠道细菌种类,并验证了它们与 HE 病理生理学相关的功能。针对这些细菌可能是治疗 HE 的一种潜在有效策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6b1c/9315133/d761f3a5b04d/HEP4-6-2090-g003.jpg

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