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巴雷特食管的细胞起源及其干细胞。

The Cellular Origin of Barrett's Esophagus and Its Stem Cells.

机构信息

McGovern Medical School, University of Texas Health Science Center in Houston, Houston, TX, USA.

Department of Biology and Biochemistry, University of Houston, Houston, TX, USA.

出版信息

Adv Exp Med Biol. 2019;1123:55-69. doi: 10.1007/978-3-030-11096-3_5.

Abstract

The incidence of esophageal adenocarcinoma is rapidly increasing in Western countries. This is despite the introduction of sophisticated endoscopic techniques and our ability to readily monitor the presumed precursor lesion known as Barrett's esophagus. Preemptive approaches, including radiofrequency ablation (RFA), and photodynamic therapy (PDT) for Barrett's esophagus and dysplasia are achieving dramatic initial results. Although the long-term efficacy of these nonspecific ablative therapies is awaiting longitudinal studies, reports of recurrences are increasing. More targeted therapies, particularly directed at the stem cells of Barrett's esophagus, demand knowing the origin of this intestinal metaplasia (IM). The prevailing concept holds that Barrett's esophagus arises from the "transcommitment" of esophageal stem cells to produce an intestine-like epithelium. An alternative explanation derives from the discovery of a discrete population of residual embryonic cells (RECs) existing at the gastroesophageal junction in normal individuals that expands and colonizes regions of the esophagus denuded by chronic reflux. These RECs form IM within days of esophageal injury, suggesting a novel mechanism of tumorigenesis.A corollary of this work is that the Barrett's stem cell is distinct from that of the squamous epithelium and, once identified, will form the basis of new preemptive strategies for addressing Barrett's and its related neoplasia.

摘要

食管腺癌在西方国家的发病率正在迅速上升。尽管我们已经引入了复杂的内镜技术,并能够轻易监测到被认为是前驱病变的 Barrett 食管,但这并没有改变这种情况。针对 Barrett 食管和异型增生的预防性方法,包括射频消融(RFA)和光动力疗法(PDT),已经取得了显著的初步效果。虽然这些非特异性消融疗法的长期疗效还需要进行纵向研究,但复发的报告正在增加。更具针对性的治疗方法,特别是针对 Barrett 食管的干细胞,需要了解这种肠化生(IM)的起源。目前占主导地位的观点认为,Barrett 食管是由食管干细胞的“转分化”产生的,类似于肠道的上皮细胞。另一种解释源自于在正常个体的胃食管交界处发现的一个离散的胚胎细胞(RECs)群体,这些细胞在慢性反流导致的食管区域裸露时会扩张并定植。这些 RECs 在食管损伤后几天内形成 IM,提示了一种新的肿瘤发生机制。这项工作的一个推论是,Barrett 干细胞与鳞状上皮的干细胞不同,一旦被识别,将成为 Barrett 及其相关肿瘤的新的预防性策略的基础。

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