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II型转化生长因子β受体在肠道细胞系和肠道中的表达

Type II TGF(beta) receptor expression in intestinal cell lines and in the intestinal tract.

作者信息

Winesett M P, Ramsey G W, Barnard J A

机构信息

Department of Pediatrics, Division of Gastroenterology and Nutrition, Vanderbilt University School of Medicine, Nashville, TN 37232-2576, USA.

出版信息

Carcinogenesis. 1996 May;17(5):989-95. doi: 10.1093/carcin/17.5.989.

Abstract

The recent identification and cloning of mammalian transforming growth factor beta (TGFbeta) receptors permits further analysis of the importance of the TGFbeta family in intestinal biology. Expression of the type II TGFbeta receptor was examined in gastrointestinal cell lines and tissues. The 5.5 kb type II mRNA species was detected in poly-(A) mRNA isolated from the rat small bowel and colon. Northern blot analysis of RNA isolated from epithelial and non-epithelial small intestinal cell fractions showed the majority of receptor mRNA localized in the non-epithelial compartment. Immunohistochemical localization in the small intestine and colon supported the RNA findings; that is, expression was greatest in the lamina propria and muscularis. Staining was also detectable in the epithelium, where it was most prominent in the villus tip cells and absent in crypt cells. These findings mirror expression of TGFbeta in the epithelial compartment. The IEC-6, IPEC and RIE-1 cell lines, all of which are non-transformed, were growth inhibited by TGFbeta and expressed type II receptor mRNA and protein. By contrast, the ras-transfected RIE-1, HT-29, Caco-2 and SW-620 transformed lines were not growth inhibited by TGFbeta and all demonstrated a marked reduction in type II TGFbeta receptor mRNA expression and protein abundance by cross-linking. In conclusion, (i) colocalization of both ligand and receptor establishes the existence of potential autocrine and/or paracrine pathways for TGFbeta in the normal intestine and (ii) down-regulation of the type II TGFbeta receptor occurs in association with cellular transformation and may contribute to intestinal carcinogenesis.

摘要

近期对哺乳动物转化生长因子β(TGFβ)受体的鉴定和克隆,使得对TGFβ家族在肠道生物学中的重要性能够进行进一步分析。对II型TGFβ受体在胃肠道细胞系和组织中的表达进行了检测。在从大鼠小肠和结肠分离的多聚腺苷酸(poly - A)mRNA中检测到了5.5 kb的II型mRNA。对从小肠上皮和非上皮细胞组分中分离的RNA进行的Northern印迹分析表明,大部分受体mRNA定位于非上皮区室。小肠和结肠中的免疫组织化学定位结果支持了RNA研究结果;也就是说,在固有层和肌层中表达最强。在上皮中也可检测到染色,在绒毛顶端细胞中最为明显,而在隐窝细胞中则不存在。这些发现反映了TGFβ在上皮区室中的表达情况。IEC - 6、IPEC和RIE - 1细胞系均未发生转化,它们的生长受到TGFβ抑制,并表达II型受体mRNA和蛋白。相比之下,经ras转染的RIE - 1、HT - 29、Caco - 2和SW - 620转化细胞系不受TGFβ抑制生长,并且通过交联显示II型TGFβ受体mRNA表达和蛋白丰度均显著降低。总之,(i)配体和受体的共定位证实了正常肠道中TGFβ潜在自分泌和/或旁分泌途径的存在,以及(ii)II型TGFβ受体的下调与细胞转化相关,可能促成肠道癌变。

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