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癌细胞与 I 型胶原黏附诱导的上皮-间充质转化。

Epithelial-Mesenchymal Transition Induced in Cancer Cells by Adhesion to Type I Collagen.

机构信息

Nippi Research Institute of Biomatrix, Ibaraki 302-0017, Japan.

Anatomy and Cell Biology, Faculty of Medicine, Osaka Medical and Pharmaceutical University, Osaka 569-8686, Japan.

出版信息

Int J Mol Sci. 2022 Dec 22;24(1):198. doi: 10.3390/ijms24010198.

Abstract

The epithelial-mesenchymal transition (EMT) is an important biological process that is physiologically observed during development, wound healing, and cancer invasion. During EMT induction, cancer cells lose their epithelial properties owing to various tumor microenvironmental factors and begin to exhibit mesenchymal properties, such as loss of apical-basal polarity, weakened intercellular adhesion, and promotion of single cell migration. Several factors, including growth factor stimulation and adhesion to type I collagen (Col-I), induce EMT in cancer cells. Cells adhere to Col-I via specific receptors and induce EMT by activating outside-in signals. In vivo, Col-I molecules often form fibrils, which then assemble into supramolecular structures (gel form). Col-I also self-assembles in vitro under physiological conditions. Notably, Col-I can be used as a culture substrate in both gel and non-gel forms, and the gel formation state of Col-I affects cell fate. Although EMT can be induced in both forms of Col-I, the effects of gel formation on EMT induction remain unclear and somewhat inconsistent. Therefore, this study reviews the relationship between Col-I gel-forming states and EMT induction in cancer cells.

摘要

上皮-间充质转化(EMT)是一种重要的生物学过程,在发育、创伤愈合和癌症侵袭过程中都有生理性观察。在 EMT 诱导过程中,由于各种肿瘤微环境因素的影响,癌细胞失去上皮特性,开始表现出间充质特性,如顶端-基底极性丧失、细胞间黏附力减弱以及促进单细胞迁移。多种因素,包括生长因子刺激和对 I 型胶原(Col-I)的黏附,诱导癌细胞发生 EMT。细胞通过特定的受体黏附在 Col-I 上,并通过激活外向信号诱导 EMT。在体内,Col-I 分子通常形成纤维,然后组装成超分子结构(凝胶形式)。Col-I 在体外也能在生理条件下自组装。值得注意的是,Col-I 可同时作为凝胶和非凝胶形式的培养底物,Col-I 的凝胶形成状态影响细胞命运。虽然 EMT 可在 Col-I 的这两种形式中被诱导,但凝胶形成对 EMT 诱导的影响尚不清楚,且存在一定的不一致性。因此,本研究综述了 Col-I 凝胶形成状态与癌细胞 EMT 诱导之间的关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f14e/9820580/d9e87d5535b7/ijms-24-00198-g001.jpg

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