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肠道稳态和结直肠癌中的信号通路:KRAS 处于中心舞台。

Signaling pathways in intestinal homeostasis and colorectal cancer: KRAS at centre stage.

机构信息

School of Medicine, Systems Biology Ireland, and UCD Charles Institute of Dermatology, University College Dublin, Belfield, Dublin 4, Ireland.

出版信息

Cell Commun Signal. 2021 Mar 10;19(1):31. doi: 10.1186/s12964-021-00712-3.

Abstract

The intestinal epithelium acts as a physical barrier that separates the intestinal microbiota from the host and is critical for preserving intestinal homeostasis. The barrier is formed by tightly linked intestinal epithelial cells (IECs) (i.e. enterocytes, goblet cells, neuroendocrine cells, tuft cells, Paneth cells, and M cells), which constantly self-renew and shed. IECs also communicate with microbiota, coordinate innate and adaptive effector cell functions. In this review, we summarize the signaling pathways contributing to intestinal cell fates and homeostasis functions. We focus especially on intestinal stem cell proliferation, cell junction formation, remodelling, hypoxia, the impact of intestinal microbiota, the immune system, inflammation, and metabolism. Recognizing the critical role of KRAS mutants in colorectal cancer, we highlight the connections of KRAS signaling pathways in coordinating these functions. Furthermore, we review the impact of KRAS colorectal cancer mutants on pathway rewiring associated with disruption and dysfunction of the normal intestinal homeostasis. Given that KRAS is still considered undruggable and the development of treatments that directly target KRAS are unlikely, we discuss the suitability of targeting pathways downstream of KRAS as well as alterations of cell extrinsic/microenvironmental factors as possible targets for modulating signaling pathways in colorectal cancer. Video Abstract.

摘要

肠道上皮作为物理屏障,将肠道微生物群与宿主隔开,对于维持肠道内稳态至关重要。屏障由紧密相连的肠道上皮细胞(IEC)(即肠上皮细胞、杯状细胞、神经内分泌细胞、微绒毛细胞、潘氏细胞和 M 细胞)组成,这些细胞不断自我更新和脱落。IEC 还与微生物群进行通信,协调先天和适应性效应细胞功能。在这篇综述中,我们总结了参与肠道细胞命运和内稳态功能的信号通路。我们特别关注肠道干细胞增殖、细胞连接形成、重塑、缺氧、肠道微生物群的影响、免疫系统、炎症和代谢。鉴于 KRAS 突变体在结直肠癌中的关键作用,我们强调了 KRAS 信号通路在协调这些功能方面的联系。此外,我们还回顾了 KRAS 结直肠癌突变体对与正常肠道内稳态破坏和功能障碍相关的通路重排的影响。鉴于 KRAS 仍被认为是不可成药的,并且不太可能开发直接针对 KRAS 的治疗方法,我们讨论了靶向 KRAS 下游通路以及改变细胞外/微环境因素作为调节结直肠癌信号通路的可能靶点的适宜性。视频摘要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2ccc/7945333/1f5467188884/12964_2021_712_Fig1_HTML.jpg

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