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分泌黏液的胃上皮祖细胞成熟为分泌消化酶的酶原细胞需要Mist1。

The maturation of mucus-secreting gastric epithelial progenitors into digestive-enzyme secreting zymogenic cells requires Mist1.

作者信息

Ramsey Victoria G, Doherty Jason M, Chen Christopher C, Stappenbeck Thaddeus S, Konieczny Stephen F, Mills Jason C

机构信息

Department of Pathology and Immunology, Washington University School of Medicine, St Louis, MO 63110, USA.

出版信息

Development. 2007 Jan;134(1):211-22. doi: 10.1242/dev.02700.

Abstract

Continuous regeneration of digestive enzyme (zymogen)-secreting chief cells is a normal aspect of stomach function that is disrupted in precancerous lesions (e.g. metaplasias, chronic atrophy). The cellular and genetic pathways that underlie zymogenic cell (ZC) differentiation are poorly understood. Here, we describe a gene expression analysis of laser capture microdissection purified gastric cell populations that identified the bHLH transcription factor Mist1 as a potential ZC regulatory factor. Our molecular and ultrastructural analysis of proliferation, migration and differentiation of the gastric unit in Mist1(-/-) and control mice supports a model whereby wild-type ZC progenitors arise as neck cells in the proliferative (isthmal) zone of the gastric unit and become transitional cells (TCs) with molecular and ultrastructural characteristics of both enzyme-secreting ZCs and mucus-secreting neck cells as they migrate to the neck-base zone interface. Thereafter, they rapidly differentiate into mature ZCs as they enter the base. By contrast, Mist1(-/-) neck cells differentiate normally, but ZCs in the mature, basal portion of the gastric unit uniformly exhibit multiple apical cytoplasmic structural abnormalities. This defect in terminal ZC differentiation is also associated with markedly increased abundance of TCs, especially in late-stage TCs that predominantly have features of immature ZCs. Thus, we present an in vivo system for analysis of ZC differentiation, present molecular evidence that ZCs differentiate from neck cell progenitors and identify Mist1 as the first gene with a role in this clinically important process.

摘要

分泌消化酶(酶原)的主细胞持续再生是胃功能的一个正常方面,而在癌前病变(如化生、慢性萎缩)中会受到破坏。对生酶细胞(ZC)分化的细胞和遗传途径了解甚少。在此,我们描述了对激光捕获显微切割纯化的胃细胞群体进行的基因表达分析,该分析确定bHLH转录因子Mist1是一种潜在的ZC调节因子。我们对Mist1基因敲除小鼠和对照小鼠胃单位增殖、迁移和分化的分子及超微结构分析支持了这样一个模型:野生型ZC祖细胞作为胃单位增殖(峡部)区的颈部细胞出现,并在迁移至颈部 - 基部区域界面时成为具有分泌酶的ZC和分泌黏液的颈部细胞分子及超微结构特征的过渡细胞(TCs)。此后,它们在进入基部时迅速分化为成熟的ZC。相比之下,Mist1基因敲除小鼠的颈部细胞正常分化,但胃单位成熟基部的ZC均表现出多个顶端细胞质结构异常。终末ZC分化的这种缺陷还与TCs丰度显著增加有关,尤其是在主要具有未成熟ZC特征的晚期TCs中。因此,我们提出了一个用于分析ZC分化的体内系统,提供了ZC从颈部细胞祖细胞分化而来的分子证据,并确定Mist1是在这一具有临床重要性的过程中发挥作用的首个基因。

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