肠道生态失调、抗增殖蛋白和转录后调控在癌变中的作用

Haruka Sawamura, Kurumi Taniguchi, Yuka Ikeda, Ai Tsuji, Y. Kitagishi, S. Matsuda
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引用次数: 1

摘要

微生物群潜在的强大影响引起了人们的广泛关注。例如,肠道菌群失调可能与各种癌症有关。肠道生态失调引起的炎症引起的DNA损伤和DNA修复损伤可能在致癌和/或预防致癌中起重要作用。事实上,在几种癌症中,肠道微生物组的特征已被证明与某些免疫阻断疗法的反应和/或成功生存率有关。相反,活细胞必须应对活性氧(ROS)破坏生物分子完整性的危险,如果不及时治疗,最终可能导致致癌。肠道微生物群可以调节相当水平的活性氧和氧化损伤。有趣的是,一个由多个即时早期反应基因产物组成的抗增殖家族(anti- prolifative family, APRO)可能深入参与了肿瘤的发生机制。已有研究表明,APRO蛋白还参与多种细胞过程,包括细胞分裂、DNA修复和mRNA稳定性。APRO蛋白的生物学功能似乎相当复杂;然而,它们可能是microrna (mirna)转录后调控的关键调节剂。下一代疗法可能包含改变氧化还原背景的策略,以及细胞中ROS的调节和/或通过以可持续的方式调节mirna衍生的转录后调节,使APRO蛋白具有更好的DNA修复机制。鉴于肠道微生物群在平衡免疫网络中的重要功能,因此,适当的肠道微生物群可以通过APRO蛋白的作用来预防致癌。因此,益生菌可能在调节肠道免疫系统以保持健康和/或预防癌症方面发挥关键作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Roles of gut dysbiosis, anti-proliferative proteins, and post-transcriptional regulation in carcinogenesis
The potentially powerful impact of microbiota has attracted much attention. For example, dysbiosis of the gut microbiota could be linked to various cancers. It is probable that DNA damage and DNA repair impairment due to inflammation from gut dysbiosis would be of importance in carcinogenesis and/or preventing carcinogenesis. In fact, the signature of the gut microbiome has been shown to be associated with responses and/or successful survival rate to certain immune-blockade therapy in several cancers. Conversely, living cells have to cope with the danger of reactive oxygen species (ROS) disturbing the integrity of biomolecules, which can eventually lead to carcinogenesis if otherwise untreated. Gut microbiota could modulate considerable levels of ROS and oxidative damage. Interestingly, an anti-proliferative family (APRO) characterized by several immediate early responsive gene products might be deeply involved in the mechanism of carcinogenesis. It has been described that APRO proteins also participate in a variety of cellular processes including cell division, DNA repair, and mRNA stability. The biological function of APRO proteins seems to be quite complicated; however, they might be a key modulator of microRNAs (miRNAs) for post-transcriptional regulation. The next generation of therapy would likely contain strategies for modifying the redox background as well as the regulation of ROS in cells and/or for better DNA repair machinery with the APRO proteins via the modulation of miRNA-derived post-transcriptional regulation in a sustainable manner. Given the important function of the gut microbiota in balancing the immune network, carcinogenesis could therefore be prevented by suitable gut microbiota via the roles of APRO proteins. Consequently, probiotics might play a key role in the modulation of gut immune system in keeping healthy and/or preventing cancers.
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