Department of Chemistry and Chemical Biology, Harvard University, 12 Oxford Street, Cambridge, MA 02138, USA.
Masonic Cancer Center, University of Minnesota, 2231 Sixth Street Southeast, Minneapolis, MN 55455, USA.
Science. 2019 Feb 15;363(6428). doi: 10.1126/science.aar7785.
Certain strains residing in the human gut produce colibactin, a small-molecule genotoxin implicated in colorectal cancer pathogenesis. However, colibactin's chemical structure and the molecular mechanism underlying its genotoxic effects have remained unknown for more than a decade. Here we combine an untargeted DNA adductomics approach with chemical synthesis to identify and characterize a covalent DNA modification from human cell lines treated with colibactin-producing Our data establish that colibactin alkylates DNA with an unusual electrophilic cyclopropane. We show that this metabolite is formed in mice colonized by colibactin-producing and is likely derived from an initially formed, unstable colibactin-DNA adduct. Our findings reveal a potential biomarker for colibactin exposure and provide mechanistic insights into how a gut microbe may contribute to colorectal carcinogenesis.
某些存在于人类肠道内的菌株会产生肠菌素,这是一种小分子遗传毒素,与结直肠癌的发病机制有关。然而,肠菌素的化学结构及其遗传毒性作用的分子机制在十多年来一直不为人知。在这里,我们结合非靶向 DNA 加合物组学方法和化学合成,鉴定并表征了用产生肠菌素的菌株处理的人细胞系中的一种共价 DNA 修饰物。我们的数据表明,肠菌素用一种不寻常的亲电环丙烷烷基化 DNA。我们表明,这种代谢物是在产生肠菌素的小鼠结肠中形成的,可能来自最初形成的不稳定的肠菌素-DNA 加合物。我们的发现揭示了肠菌素暴露的一个潜在生物标志物,并提供了关于肠道微生物如何促成结直肠癌发生的机制见解。
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