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胎儿结肠、皮肤和胆管上皮细胞中独特共同表位的同时出现。溃疡性结肠炎肠外表现的一种可能联系。

Simultaneous appearance of a unique common epitope in fetal colon, skin, and biliary epithelial cells. A possible link for extracolonic manifestations in ulcerative colitis.

作者信息

Das K M, Squillante L, Chitayet D, Kalousek D K

机构信息

University of Medicine and Dentistry-Robert Wood Johnson Medical School, New Brunswick, New Jersey 08903.

出版信息

J Clin Gastroenterol. 1992 Dec;15(4):311-6. doi: 10.1097/00004836-199212000-00009.

Abstract

The tissue distribution of a previously identified M(r) 40 K epithelial autoantigen in ulcerative colitis was examined in situ in the fetal tissue by immunocytochemical method, using an immunoglobulin M (IgM) monoclonal antibody (7E12H12). Fetal-autopsy tissue from 9 to 19 weeks of development (11-21 gestational weeks) gestations, including specimens of colon (20 specimens), skin (19), small intestine (12), gallbladder (15), liver (20), spleen (20), kidney (3), urinary bladder (3), and umbilical cord/placenta (25) were examined. 7E12H12 reactive epitope appeared first in a few colonic epithelial cells at 10 weeks of gestation. By 11 weeks, 7E12H12 reactivity was clearly evident in most of the colonic epithelial cells. Goblet-cell reactivity was evident from 15 weeks of gestation. Enterocytes lining the small intestine from all the specimens were negative. In the skin, earliest immunoreactivity was evident in the basal layer of epidermis at 10 weeks of development, and by 11 weeks, the staining was intense and localized exclusively to squamous epithelial cells of the epidermis. The immunoreactivity in the fetal gallbladder mucosa was also evident earliest at 11 weeks of development. The staining was distinct in the mucosal epithelial cells, and localized along the periphery of the cells and in the apical areas. None of the other tissue specimens reacted with 7E12H12. These results demonstrate that the 7E12H12 reactive epitope is novel, is shared by colon, skin, and biliary epithelium, and appears more or less simultaneously in the three organs at 10 to 11 weeks of development of the fetus. A possible link of this crossreactive protein or proteins in the immunopathogenesis of ulcerative colitis, sclerosing cholangitis, and pyoderma gangrenosum is discussed.

摘要

采用免疫细胞化学方法,使用免疫球蛋白M(IgM)单克隆抗体(7E12H12),在原位对胎儿组织中先前鉴定的分子量为40kDa的上皮自身抗原在溃疡性结肠炎中的组织分布进行了检测。对9至19周发育阶段(妊娠11至21周)的胎儿尸检组织进行了检查,包括结肠标本(20份)、皮肤(19份)、小肠(12份)、胆囊(15份)、肝脏(20份)、脾脏(20份)、肾脏(3份)、膀胱(3份)以及脐带/胎盘(25份)。7E12H12反应性表位在妊娠10周时首先出现在少数结肠上皮细胞中。到11周时,7E12H12反应性在大多数结肠上皮细胞中明显可见。杯状细胞反应性从妊娠15周开始明显。所有标本中小肠的肠上皮细胞均为阴性。在皮肤中,最早的免疫反应性在发育10周时出现在表皮基底层,到11周时,染色强烈且仅局限于表皮的鳞状上皮细胞。胎儿胆囊黏膜中的免疫反应性最早在发育11周时也明显可见。染色在黏膜上皮细胞中明显,沿细胞周边和顶端区域定位。其他组织标本均未与7E12H12发生反应。这些结果表明,7E12H12反应性表位是新的,在结肠、皮肤和胆管上皮中共有,并且在胎儿发育10至11周时在这三个器官中或多或少同时出现。讨论了这种交叉反应蛋白或多种蛋白在溃疡性结肠炎、硬化性胆管炎和坏疽性脓皮病免疫发病机制中的可能联系。

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