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通过培养依赖和非培养依赖研究推断出人肠道微生物组中抗癌 Azurin 编码和 Azurin 样基因的分子筛选和遗传多样性分析。

Molecular screening and genetic diversity analysis of anticancer Azurin-encoding and Azurin-like genes in human gut microbiome deduced through cultivation-dependent and cultivation-independent studies.

机构信息

Institute of Biotechnology and Environment, Nha Trang University, Nha Trang, Vietnam.

School of Engineering, Cardiff University, Cardiff, UK.

出版信息

Int Microbiol. 2019 Dec;22(4):437-449. doi: 10.1007/s10123-019-00070-8. Epub 2019 Mar 20.

DOI:10.1007/s10123-019-00070-8
PMID:30895406
Abstract

Azurin, a bacteriocin produced by a human gut bacterium Pseudomonas aeruginosa, can reveal selectively cytotoxic and induce apoptosis in cancer cells. After overcoming two phase I trials, a functional region of Azurin called p28 has been approved as a drug for the treatment of brain tumor glioma by FDA. The present study aims to improve a screening procedure and assess genetic diversity of Azurin genes in P. aeruginosa and Azurin-like genes in the gut microbiome of a specific population in Vietnam and global populations. Firstly, both cultivation-dependent and cultivation-independent techniques based on genomic and metagenomic DNAs extracted from fecal samples of the healthy specific population were performed and optimized to detect Azurin genes. Secondly, the Azurin gene sequences were analyzed and compared with global populations by using bioinformatics tools. Finally, the screening procedure improved from the first step was applied for screening Azurin-like genes, followed by the protein synthesis and NCI in vitro screening for anticancer activity. As a result, this study has successfully optimized the annealing temperatures to amplify DNAs for screening Azurin genes and applying to Azurin-like genes from human gut microbiota. The novelty of this study is the first of its kind to classify Azurin genes into five different genotypes at a global scale and confirm the potential anticancer activity of three Azurin-like synthetic proteins (Cnazu1, Dlazu11, and Ruazu12). The results contribute to the procedure development applied for screening anticancer proteins from human microbiome and a comprehensive understanding of their therapeutic response at a genetic level.

摘要

蓝铜蛋白是一种由人类肠道细菌铜绿假单胞菌产生的细菌素,能够选择性地杀伤癌细胞并诱导其凋亡。经过两项 I 期临床试验,蓝铜蛋白的一个功能区域 p28 已被 FDA 批准为治疗脑肿瘤胶质母细胞瘤的药物。本研究旨在改进一种筛选程序,并评估越南特定人群肠道微生物组中铜绿假单胞菌和蓝铜蛋白样基因的遗传多样性。首先,基于从健康特定人群粪便样本中提取的基因组和宏基因组 DNA,进行了培养依赖和非培养依赖的技术,并对其进行了优化,以检测蓝铜蛋白基因。其次,利用生物信息学工具对蓝铜蛋白基因序列进行分析和比较,并与全球人群进行比较。最后,将第一步中改进的筛选程序应用于筛选蓝铜蛋白样基因,然后进行蛋白质合成和 NCI 体外筛选抗癌活性。结果表明,本研究成功优化了用于筛选蓝铜蛋白基因的退火温度,并将其应用于人类肠道微生物组中的蓝铜蛋白样基因。本研究的新颖之处在于,首次在全球范围内将蓝铜蛋白基因分为五种不同的基因型,并证实了三种合成蓝铜蛋白样蛋白(Cnazu1、Dlazu11 和 Ruazu12)的潜在抗癌活性。研究结果有助于开发从人类微生物组中筛选抗癌蛋白的程序,并从遗传水平全面了解其治疗反应。

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