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Cadherin adhesion in the intestinal crypt regulates morphogenesis, mitogenesis, motogenesis, and metaplasia formation.

机译:钙离子粘附在肠隐窝中可调节形态发生,有丝分裂,运动发生和化生形成。

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摘要

The topographical organisation of the epithelium lining mucous membranes has been an intense point of research. One of the fundamental biological issues underpinning this and associated issues relates to the role and regulation of epithelial adhesion molecules. Adhesion between individual cells allows an intact layer to be formed, which is selectively permeable. In addition, the orchestrated regulation of multiple adhesion molecules allows the gradual transition from basal secretory cells to apical absorptive cells in the crypt-villus gradient. Moreover, it is becoming clear that no one class of adhesion molecule can sufficiently govern crypt architecture; however, the main cell-cell adhesion molecules are the cadherins and the related desmosomal cadherins. These latter molecules interact with the catenins, which bind directly or indirectly with cytoskeletal molecules such as Rho and Rac. In addition, other complex glycoproteins, such as the carcinoembryonic antigens, might contribute to adhesion, although their mechanisms of function are distinctly different. Integrins on the basal aspect of the cells also signal important morphoregulatory signals as a result of their binding to the extracellular maxtrix. The disruption of these physiological processes also provides a necessary and, in some cases, sufficient molecular mechanism for cancer invasion and metastasis, such as occurs in E-cadherin mutation positive familial gastric cancer.
机译:上皮内衬粘膜的地形组织一直是研究的重点。支撑该现象和相关问题的基本生物学问题之一涉及上皮粘附分子的作用和调节。各个单元之间的粘附力可形成完整的层,该层是可选择性渗透的。另外,多种粘附分子的协调调节允许隐窝-绒毛梯度中从基底分泌细胞逐渐过渡到根尖吸收细胞。而且,越来越明显的是,没有一种粘附分子能够充分控制隐窝结构。然而,主要的细胞-细胞粘附分子是钙粘蛋白和相关的桥粒钙粘蛋白。后面这些分子与连环蛋白相互作用,连环蛋白直接或间接与细胞骨架分子(如Rho和Rac)结合。此外,其他复杂的糖蛋白,例如癌胚抗原,可能会促进粘附,尽管它们的功能机制明显不同。由于细胞与细胞外基质结合,整合素在细胞的基础方面也发出重要的形态调节信号。这些生理过程的破坏还为癌症的侵袭和转移提供了必要且在某些情况下足够的分子机制,例如发生在E-钙粘蛋白突变阳性的家族性胃癌中。

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