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Transitional basal cells at the squamous-columnar junction generate Barrett’s oesophagus

机译:鳞状-柱状交界处的过渡基底细胞产生巴雷特食管

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摘要

In several organ systems the transitional zone between different types of epithelia is a hotspot for pre-neoplastic metaplasia and malignancy. However, the cell-of-origin for the metaplastic epithelium and subsequent malignancy, remains obscure. In the case of Barrett’s oesophagus (BE), intestinal metaplasia occurs at the gastro-oesophageal junction, where stratified squamous epithelium transitions into simple columnar cells. Based on different experimental models, several alternative cell types have been proposed as the source of the metaplasia, but in all cases the evidence is inconclusive and no model completely mimics BE with the presence of intestinal goblet cells. Here, we describe a novel transitional columnar epithelium with distinct basal progenitor cells (p63+ KRT5+ KRT7+) in the squamous-columnar junction (SCJ) in the upper gastrointestinal tract of the mouse. We use multiple models and lineage tracing strategies to show that this unique SCJ basal cell population serves as a source of progenitors for the transitional epithelium. Moreover, upon ectopic expression of CDX2 these transitional basal progenitors differentiate into intestinal-like epithelium including goblet cells, thus reproducing Barrett’s metaplasia. A similar transitional columnar epithelium is present at the transitional zones of other mouse tissues, including the anorectal junction, and, importantly, at the gastro-oesophageal junction in the human gut. Acid reflux-induced oesophagitis and the multilayered epithelium (MLE) believed to be a precursor of BE are both characterized by the expansion of the transitional basal progenitor cells. Taken together our findings reveal the presence of a previously unidentified transitional zone in the epithelium of the upper gastrointestinal tract and provide evidence that the p63+ KRT7+ basal cells in this zone are the cell-of-origin for MLE and BE.
机译:在几个器官系统中,不同类型的上皮之间的过渡区是肿瘤前化生和恶性肿瘤的热点。但是,化生上皮和随后的恶性肿瘤的起源细胞仍然是晦涩的。就Barrett食道(BE)而言,肠上皮化生发生在胃食管连接处,分层的鳞状上皮细胞转变为简单的柱状细胞 。基于不同的实验模型,已经提出了几种替代的细胞类型作为化生的来源,但是在所有情况下,证据尚无定论,并且没有模型完全模仿存在肠杯状细胞的BE。在这里,我们描述了一种新的过渡性柱状上皮,在鳞状-柱状交界处具有不同的基础祖细胞(p63 + KRT5 + KRT7 + ) SCJ)在小鼠的上消化道中。我们使用多种模型和谱系追踪策略来表明,这种独特的SCJ基底细胞群可作为过渡上皮祖细胞的来源。此外,在异位表达CDX2时,这些过渡性基础祖细胞分化为包括杯状细胞的肠样上皮,从而重现Barrett的化生。类似的过渡柱状上皮存在于其他小鼠组织的过渡区,包括肛门直肠交界处,并且重要的是,在人肠的胃-食道交界处。酸性反流性食管炎和多层上皮(MLE)被认为是BE的前体,均以过渡性基础祖细胞的扩增为特征。综上所述,我们的发现揭示了在上消化道上皮中存在一个先前未知的过渡区,并提供了证据表明该区的p63 + KRT7 + 基底细胞是MLE和BE的原点细胞。

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