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泰国结直肠息肉患者独特的肠道微生物群。

Distinct gut microbiomes in Thai patients with colorectal polyps.

作者信息

Intarajak Thoranin, Udomchaiprasertkul Wandee, Khoiri Ahmad Nuruddin, Sutheeworapong Sawannee, Kusonmano Kanthida, Kittichotirat Weerayuth, Thammarongtham Chinae, Cheevadhanarak Supapon

机构信息

Bioinformatics Unit, Chulabhorn Royal Academy, Lak Si 10210, Bangkok, Thailand.

Bioinformatics and Systems Biology Program, School of Bioresources and Technology, and School of Information Technology, King Mongkut's University of Technology Thonburi, Bang Khun Thian 10150, Bangkok, Thailand.

出版信息

World J Gastroenterol. 2024 Jul 21;30(27):3336-3355. doi: 10.3748/wjg.v30.i27.3336.

Abstract

BACKGROUND

Colorectal polyps that develop the conventional adenoma-carcinoma sequence [, tubular adenoma (TA)] often progress to malignancy and are closely associated with changes in the composition of the gut microbiome. There is limited research concerning the microbial functions and gut microbiomes associated with colorectal polyps that arise through the serrated polyp pathway, such as hyperplastic polyps (HP). Exploration of microbiome alterations associated with HP and TA would improve the understanding of mechanisms by which specific microbes and their metabolic pathways contribute to colorectal carcinogenesis.

AIM

To investigate gut microbiome signatures, microbial associations, and microbial functions in HP and TA patients.

METHODS

Full-length 16S rRNA sequencing was used to characterize the gut microbiome in stool samples from control participants without polyps [control group (CT), = 40], patients with HP ( = 52), and patients with TA ( = 60). Significant differences in gut microbiome composition and functional mechanisms were identified between the CT group and patients with HP or TA. Analytical techniques in this study included differential abundance analysis, co-occurrence network analysis, and differential pathway analysis.

RESULTS

Colorectal cancer (CRC)-associated bacteria, including (), , and , were identified as characteristic microbial species in TA patients. associated with dysbiosis and gastrointestinal diseases, was significantly differentially abundant in the HP and TA groups. Functional pathway analysis revealed that HP patients exhibited enrichment in the sulfur oxidation pathway exclusively, whereas TA patients showed dominance in pathways related to secondary metabolite biosynthesis (, mevalonate); was a major contributor. Co-occurrence network and dynamic network analyses revealed co-occurrence of dysbiosis-associated bacteria in HP patients, whereas TA patients exhibited co-occurrence of CRC-associated bacteria. Furthermore, the co-occurrence of SCFA-producing bacteria was lower in TA patients than HP patients.

CONCLUSION

This study revealed distinct gut microbiome signatures associated with pathways of colorectal polyp development, providing insights concerning the roles of microbial species, functional pathways, and microbial interactions in colorectal carcinogenesis.

摘要

背景

发生传统腺瘤 - 癌序列(如管状腺瘤(TA))的大肠息肉通常会进展为恶性肿瘤,并且与肠道微生物群组成的变化密切相关。关于通过锯齿状息肉途径产生的大肠息肉(如增生性息肉(HP))相关的微生物功能和肠道微生物群的研究有限。探索与HP和TA相关的微生物群改变将有助于更好地理解特定微生物及其代谢途径促进结直肠癌发生的机制。

目的

研究HP和TA患者的肠道微生物群特征、微生物关联及微生物功能。

方法

采用全长16S rRNA测序对无息肉对照参与者(对照组(CT),n = 40)、HP患者(n = 52)和TA患者(n = 60)粪便样本中的肠道微生物群进行表征。确定CT组与HP或TA患者之间肠道微生物群组成和功能机制的显著差异。本研究中的分析技术包括差异丰度分析、共现网络分析和差异途径分析。

结果

在TA患者中,鉴定出与结直肠癌(CRC)相关的细菌,包括()、和,为特征性微生物物种。与生态失调和胃肠道疾病相关的,在HP和TA组中差异显著丰富。功能途径分析显示,HP患者仅在硫氧化途径中富集,而TA患者在与次生代谢物生物合成相关的途径(如甲羟戊酸)中占主导地位;是主要贡献者。共现网络和动态网络分析显示,HP患者中存在与生态失调相关细菌的共现,而TA患者中存在与CRC相关细菌的共现。此外,TA患者中产生短链脂肪酸的细菌的共现低于HP患者。

结论

本研究揭示了与大肠息肉发展途径相关的独特肠道微生物群特征,为微生物物种、功能途径和微生物相互作用在结直肠癌发生中的作用提供了见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/48c3/11287419/0bc7c155a066/WJG-30-3336-g001.jpg

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