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From gut homeostasis to cancer.

机译:从肠道稳态到癌症。

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摘要

The mammalian intestine has one of the highest turnover rates in the body. The intestinal epithelium is completely renewed in less than a week. It is divided into spatially distinct compartments in the form of finger-like projections and invaginations that are dedicated to specific functions. Intestinal cells are constantly produced from a stem cell reservoir that gives rise to proliferating transient amplifying cells, which subsequently differentiate and migrate to the correct compartment before dying after having fulfilled their physiological function. In recent years, a substantial body of evidence has accumulated to support the concept that signaling pathways known to be crucial for embryonic development of multiple organisms play a critical role in tightly regulating and controlling the self-renewing process of the intestine. Moreover, the same pathways appear to be deregulated in several hereditary and sporadic colorectal cancer syndromes due to activating and/or inactivating mutations of key components of such pathways. In this review we discuss recent findings demonstrating that differentiation and homeostasis of the intestine are controlled by developmental pathways such as Wnt, Notch, TGF-beta and Hedgehog, and illustrate how their deregulation contributes to intestinal neoplasia.
机译:哺乳动物的肠道是人体中最高的周转率之一。肠上皮在不到一周的时间内即可完全更新。它以手指状的投影和内陷的形式分为空间上不同的部分,专门用于特定功能。肠道细胞不断地从干细胞储库中产生,从而引起增殖的瞬时扩增细胞,随后它们分化并迁移到正确的区室,在完成其生理功能后死亡。近年来,已经积累了大量证据来支持这样的概念,即已知对多种生物的胚胎发育至关重要的信号通路在严格调节和控制肠的自我更新过程中起着至关重要的作用。此外,由于活化和/或失活这些途径关键成分的突变,在某些遗传性和散发性结直肠癌综合症中,相同的途径似乎被解除了调控。在这篇综述中,我们讨论了最近的发现,这些发现证明了肠的分化和体内平衡受发育途径如Wnt,Notch,TGF-beta和Hedgehog的控制,并说明了它们的失调如何促进肠道肿瘤。

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