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基于16S rRNA基因扩增子和浅层宏基因组测序技术探究结直肠疾病患者的肠道微生物群

Exploring Gut Microbiota in Patients with Colorectal Disease Based on 16S rRNA Gene Amplicon and Shallow Metagenomic Sequencing.

作者信息

Liu Yuanfeng, Li Xiang, Yang Yudie, Liu Ye, Wang Shijun, Ji Boyang, Wei Yongjun

机构信息

Department of Vascular and Endovascular Surgery, First Affiliated Hospital of Zhengzhou University, Zhengzhou, Henan, China.

Science China Press, Beijing, China.

出版信息

Front Mol Biosci. 2021 Jul 9;8:703638. doi: 10.3389/fmolb.2021.703638. eCollection 2021.

Abstract

The gastrointestinal tract, the largest human microbial reservoir, is highly dynamic. The gut microbes play essential roles in causing colorectal diseases. In the present study, we explored potential keystone taxa during the development of colorectal diseases in central China. Fecal samples of some patients were collected and were allocated to the adenoma (Group A), colorectal cancer (Group C), and hemorrhoid (Group H) groups. The 16S rRNA amplicon and shallow metagenomic sequencing (SMS) strategies were used to recover the gut microbiota. Microbial diversities obtained from 16S rRNA amplicon and SMS data were similar. Group C had the highest diversity, although no significant difference in diversity was observed among the groups. The most dominant phyla in the gut microbiota of patients with colorectal diseases were Bacteroidetes, Firmicutes, and Proteobacteria, accounting for >95% of microbes in the samples. The most abundant genera in the samples were , , and , and further species-level and network analyses identified certain potential keystone taxa in each group. Some of the dominant species, such as , , and , could be responsible for causing colorectal diseases. The SMS data recovered diverse antibiotic resistance genes of tetracycline, macrolide, and beta-lactam, which could be a result of antibiotic overuse. This study explored the gut microbiota of patients with three different types of colorectal diseases, and the microbial diversity results obtained from 16S rRNA amplicon sequencing and SMS data were found to be similar. However, the findings of this study are based on a limited sample size, which warrants further large-scale studies. The recovery of gut microbiota profiles in patients with colorectal diseases could be beneficial for future diagnosis and treatment with modulation of the gut microbiota. Moreover, SMS data can provide accurate species- and gene-level information, and it is economical. It can therefore be widely applied in future clinical metagenomic studies.

摘要

胃肠道是人体最大的微生物储存库,具有高度的动态性。肠道微生物在结直肠疾病的发生中起着至关重要的作用。在本研究中,我们探索了中国中部地区结直肠疾病发展过程中的潜在关键分类群。收集了部分患者的粪便样本,并将其分为腺瘤组(A组)、结直肠癌组(C组)和痔疮组(H组)。采用16S rRNA扩增子和浅层宏基因组测序(SMS)策略来恢复肠道微生物群。从16S rRNA扩增子和SMS数据获得的微生物多样性相似。C组的多样性最高,尽管各组之间在多样性上未观察到显著差异。结直肠疾病患者肠道微生物群中最主要的门是拟杆菌门、厚壁菌门和变形菌门,占样本中微生物的95%以上。样本中最丰富的属是 、 和 ,进一步的物种水平和网络分析确定了每组中的某些潜在关键分类群。一些优势物种,如 、 和 ,可能是导致结直肠疾病的原因。SMS数据恢复了四环素、大环内酯和β-内酰胺等多种抗生素抗性基因,这可能是抗生素过度使用的结果。本研究探索了三种不同类型结直肠疾病患者的肠道微生物群,发现从16S rRNA扩增子测序和SMS数据获得的微生物多样性结果相似。然而,本研究的结果基于有限的样本量,这需要进一步的大规模研究。恢复结直肠疾病患者的肠道微生物群谱可能有利于未来通过调节肠道微生物群进行诊断和治疗。此外,SMS数据可以提供准确的物种和基因水平信息,并且经济实惠。因此,它可以广泛应用于未来的临床宏基因组研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0d43/8299945/b8e925394d04/fmolb-08-703638-g001.jpg

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