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肠道微生物结构变化可作为替代终点,用于监测致癌物暴露引起的宿主健康变化。

Structural shifts of gut microbiota as surrogate endpoints for monitoring host health changes induced by carcinogen exposure.

机构信息

Ministry of Education Key Laboratory of Systems Biomedicine, Shanghai Center for Systems Biomedicine, Shanghai Jiao Tong University, Shanghai, China.

出版信息

FEMS Microbiol Ecol. 2010 Sep;73(3):577-86. doi: 10.1111/j.1574-6941.2010.00924.x. Epub 2010 Jul 7.

Abstract

This study monitored structural shifts of gut microbiota of rats developing precancerous mucosal lesions induced by carcinogen 1,2-dimethyl hydrazine (DMH) treatment using PCR-denaturing gradient gel electrophoresis (DGGE) and 454 pyrosequencing on the 16S rRNA gene V3 region. Partial least square discriminant analysis of DGGE fingerprints showed that the gut microbiota structure of treated animals was similar to that of the controls 1 and 3 weeks after DMH treatments, but significantly different 7 weeks after DMH treatments, when a large number of aberrant crypt foci (ACF) developed in their colons. Martens' uncertainty test, followed by anova test (P<0.05) identified Ruminococcus-like and Allobaculum-like bacteria as key variables for discrimination of DMH-treated rats from controls. Real-time PCR confirmed the significant increase of the Ruminococcus obeum and the Allobaculum-like bacteria in DMH-treated rats. UniFrac analysis based on V3 pyrosequencing further validated that the gut microbiota structures of treated and control animals were similar at an early stage, but segregated after ACF formation. Thirteen operational taxonomic units including Ruminococcus-like and Allobaculum-like bacteria were identified as key variables for the discrimination of DMH-treated rats from controls. Dynamic analysis of gut microbiota may become a noninvasive strategy for monitoring host health changes induced by carcinogen exposure.

摘要

本研究采用 PCR-变性梯度凝胶电泳(DGGE)和 16S rRNA 基因 V3 区的 454 焦磷酸测序技术,监测了致癌物 1,2-二甲基肼(DMH)处理诱导的大鼠癌前黏膜病变发展过程中肠道微生物群落结构的变化。DGGE 指纹图谱的偏最小二乘判别分析显示,DMH 处理后 1 周和 3 周时,处理动物的肠道微生物群落结构与对照组相似,但在 DMH 处理后 7 周时,大量异常隐窝病灶(ACF)出现在结肠中,其肠道微生物群落结构则与对照组有明显差异。马氏不确定度检验后,经方差分析(P<0.05)鉴定出类似于 Ruminococcus 和 Allobaculum 的细菌是区分 DMH 处理大鼠和对照组的关键变量。实时 PCR 进一步证实了 Ruminococcus obeum 和类似于 Allobaculum 的细菌在 DMH 处理大鼠中的显著增加。基于 V3 焦磷酸测序的 UniFrac 分析进一步验证了处理和对照组动物的肠道微生物群落结构在早期相似,但在 ACF 形成后分离。包括类似于 Ruminococcus 和 Allobaculum 的细菌在内的 13 个操作分类单元被鉴定为区分 DMH 处理大鼠和对照组的关键变量。肠道微生物群落的动态分析可能成为监测致癌物暴露引起的宿主健康变化的一种非侵入性策略。

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