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一种独特的多层上皮的表型特征表明,它是巴雷特食管发育过程中的前体。

Phenotypic characteristics of a distinctive multilayered epithelium suggests that it is a precursor in the development of Barrett's esophagus.

作者信息

Glickman J N, Chen Y Y, Wang H H, Antonioli D A, Odze R D

机构信息

Departments of Pathology, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

Am J Surg Pathol. 2001 May;25(5):569-78. doi: 10.1097/00000478-200105000-00002.

Abstract

A distinctive type of multilayered epithelium (ME) has been described at the neo-squamocolumnar junction and within columnar mucosa in patients with Barrett's esophagus (BE). This epithelium has morphologic and ultrastructural features of both squamous and columnar epithelium. Multilayered epithelium may represent an early or intermediate stage of columnar metaplasia; therefore, we performed this study to determine the morphologic and biologic characteristics of this epithelium and to gain insight into its derivation. Esophageal mucosal biopsies containing ME from 17 patients with BE were evaluated morphologically, stained with a variety of mucin histochemical stains; and also immunostained with antibodies against cytokeratins (CK) 13 (squamous epithelium marker); 14 (basal squamous epithelium marker) 7, 8/18, 19, and 20 (columnar epithelium markers), MIB-1 (proliferation marker); villin (intestinal brush border protein); and TGFalpha, EGFR, pS2, and hSP (enteric proliferation/differentiation regulatory peptides). The results were compared with normal esophageal squamous epithelium, normal gastric cardia epithelium, specialized-type intestinal epithelium (BE), and esophageal mucosal and submucosal gland duct epithelium. Multilayered epithelium expressed a pattern of mucin production (neutral mucin, sialomucin, and sulfomucin in 88%, 100%, and 71% of cases, respectively) and cytokeratin expression (CK 13 and 19 in the basal "squamoid" cells, CK 7, 8/18, 19, and 20 in the superficial "columnar" cells) similar to that of columnar epithelium in BE, and showed a high capacity for cellular proliferation (Ki-67-positive in 88% of cases) and differentiation (TGFalpha, EGFR, pS2 and villin-positive in 100%, 100%, 93%, and 66% of cases, respectively). The mucosal gland duct epithelium showed a similar phenotypic pattern and, in one case, was seen to give rise to ME at the surface of the mucosa. These data provide evidence in support of the hypothesis that ME represents an early or intermediate stage in the development of esophageal columnar metaplasia (BE). The mucosal gland duct epithelium may contain progenitor cells that can give rise to ME.

摘要

在巴雷特食管(BE)患者的新鳞柱状交界处和柱状黏膜内,已描述了一种独特类型的复层上皮(ME)。这种上皮具有鳞状上皮和柱状上皮的形态学及超微结构特征。复层上皮可能代表柱状化生的早期或中间阶段;因此,我们开展了本研究以确定这种上皮的形态学和生物学特征,并深入了解其起源。对17例BE患者含有ME的食管黏膜活检标本进行了形态学评估,用多种黏蛋白组织化学染色剂染色;还用抗细胞角蛋白(CK)13(鳞状上皮标志物)、14(基底鳞状上皮标志物)、7、8/18、19和20(柱状上皮标志物)、MIB-1(增殖标志物)、绒毛蛋白(肠刷状缘蛋白)以及转化生长因子α(TGFalpha)、表皮生长因子受体(EGFR)、pS2和hSP(肠增殖/分化调节肽)的抗体进行免疫染色。将结果与正常食管鳞状上皮、正常胃贲门上皮、特殊类型肠上皮(BE)以及食管黏膜和黏膜下腺导管上皮进行比较。复层上皮表达的黏蛋白产生模式(分别在88%、100%和71%的病例中表达中性黏蛋白、涎黏蛋白和硫黏蛋白)和细胞角蛋白表达模式(基底“鳞状样”细胞中表达CK 13和19,表层“柱状”细胞中表达CK 7、8/18、19和20)与BE中的柱状上皮相似,并显示出高细胞增殖能力(88%的病例中Ki-67阳性)和分化能力(分别在100%、100%、93%和66%的病例中TGFalpha、EGFR、pS2和绒毛蛋白阳性)。黏膜腺导管上皮显示出类似的表型模式,并且在1例病例中,可见其在黏膜表面产生ME。这些数据为ME代表食管柱状化生(BE)发展的早期或中间阶段这一假说提供了支持证据。黏膜腺导管上皮可能含有可产生ME的祖细胞。

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