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大肠杆菌靶向宿主细胞核蛋白的计算机模拟预测,特别涉及其在结肠癌病因学中的作用。

In silico prediction of escherichia coli proteins targeting the host cell nucleus, with special reference to their role in colon cancer etiology.

作者信息

Khan Abdul Arif

机构信息

Department of Pharmaceutics, College of Pharmacy, King Saud University , Riyadh, Saudi Arabia .

出版信息

J Comput Biol. 2014 Jun;21(6):466-75. doi: 10.1089/cmb.2014.0001. Epub 2014 Mar 10.

DOI:10.1089/cmb.2014.0001
PMID:24611522
Abstract

The potential role of Escherichia coli in the development of colorectal carcinoma (CRC) has been investigated in many studies. Although the exact mechanism is not clear, chronic inflammation caused by E. coli and other related events are suggested as possible causes behind E. coli-induced colon cancer. It has been found that CRC cells, but not normal cells, are colonized by an intracellular form of E. coli. We predicted nuclear targeting of bacterial proteins in the host cell through computational tools nuclear localization signal (NLS) mapper and balanced subcellular localization predictor (BaCeILo). During intracellular E. coli residence, such targeting is highly likely and may have a possible role in colon cancer etiology. We observed that several gene expression-associated proteins of E. coli can migrate to the host nucleus during intracellular infections. This situation provides an opportunity for competitive interaction of host and pathogen proteins with similar cellular substrates, thereby increasing the chances of development of colon cancer. Moreover, the results indicated that proteins localized in the membrane of E. coli mostly act as secretary proteins in host cells. No exact correlation was observed between NLS prediction and nuclear localization prediction by BaCeILo. This is partly because of a number of reasons, including that only 30% of nuclear proteins carry NLS and that proteins <40 kDa molecular weight can passively target the host nucleus. This study concludes that detection of gene expression-specific E. coli proteins and their targeting of the nucleus may have a profound impact on CRC etiology.

摘要

许多研究都对大肠杆菌在结直肠癌(CRC)发生发展中的潜在作用进行了调查。尽管确切机制尚不清楚,但大肠杆菌引起的慢性炎症及其他相关事件被认为是大肠杆菌诱发结肠癌的可能原因。研究发现,结直肠癌细胞而非正常细胞会被细胞内形式的大肠杆菌定植。我们通过计算工具核定位信号(NLS)映射器和平衡亚细胞定位预测器(BaCeILo)预测了宿主细胞中细菌蛋白的核靶向作用。在细胞内大肠杆菌驻留期间,这种靶向作用很可能发生,并且可能在结肠癌病因学中发挥作用。我们观察到,在细胞内感染期间,大肠杆菌的几种与基因表达相关的蛋白能够迁移到宿主细胞核。这种情况为宿主和病原体蛋白与相似细胞底物的竞争性相互作用提供了机会,从而增加了患结肠癌的几率。此外,结果表明,位于大肠杆菌膜上的蛋白在宿主细胞中大多充当分泌蛋白。NLS预测与BaCeILo的核定位预测之间未观察到确切的相关性。部分原因有很多,包括只有30%的核蛋白携带NLS,以及分子量小于40 kDa的蛋白可被动靶向宿主细胞核。本研究得出结论,检测基因表达特异性的大肠杆菌蛋白及其对细胞核的靶向作用可能对结肠癌病因学产生深远影响。

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