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具有不同黏附功能的细胞黏附分子105(Cell-CAM105)同工型在成年大鼠组织和肝脏发育过程中共同表达。

Cell-CAM105 isoforms with different adhesion functions are coexpressed in adult rat tissues and during liver development.

作者信息

Cheung P H, Thompson N L, Earley K, Culic O, Hixson D, Lin S H

机构信息

Department of Molecular Pathology, University of Texas M. D. Anderson Cancer Center, Houston 77030.

出版信息

J Biol Chem. 1993 Mar 25;268(9):6139-46.

PMID:8454589
Abstract

The rat hepatocyte cell adhesion molecule cell-CAM105 has recently been shown to be composed of at least two isoforms. Expression of the two isoforms in different tissues and during fetal liver development in rats was studied by RNase protection using a probe which could specifically and simultaneously detect both isoforms. This probe revealed protected fragments of expected lengths for the L-form and the S-form in RNA samples isolated from various adult rat tissues. High levels of the L-form and S-form messages were detected in liver and intestine, moderate levels were detected in lung, and weak signals were detected in muscle, kidney, and spleen. In liver development studies, the messages for cell-CAM105 showed a major increase on the first day after birth compared to the fetal stage, and both isoform messages were proportionally increased. These results indicate that both cell-CAM105 isoforms may have function(s) related to hepatocyte differentiation. To study the adhesion function of cell-CAM105 isoforms, full-length cDNAs for these isoforms were expressed in insect cells. The insect cells expressing the L-form cell-CAM105 were found to aggregate. However, expression of S-form cell-CAM105 did not support cell aggregation. These results indicate that L-form, but not S-form, cell-CAM105 directly mediates the cell adhesion function.

摘要

大鼠肝细胞细胞黏附分子细胞-CAM105最近被证明至少由两种亚型组成。使用一种能够特异性同时检测两种亚型的探针,通过核糖核酸酶保护法研究了这两种亚型在大鼠不同组织以及胎儿肝脏发育过程中的表达情况。该探针在从成年大鼠各种组织分离的RNA样本中揭示了L型和S型预期长度的受保护片段。在肝脏和肠道中检测到高水平的L型和S型信息,在肺中检测到中等水平,在肌肉、肾脏和脾脏中检测到微弱信号。在肝脏发育研究中,与胎儿阶段相比,出生后第一天细胞-CAM105的信息显著增加,并且两种亚型的信息都成比例增加。这些结果表明,细胞-CAM105的两种亚型可能都具有与肝细胞分化相关的功能。为了研究细胞-CAM105亚型的黏附功能,这些亚型的全长cDNA在昆虫细胞中表达。发现表达L型细胞-CAM105的昆虫细胞会聚集。然而,S型细胞-CAM105的表达不支持细胞聚集。这些结果表明,直接介导细胞黏附功能的是L型而非S型细胞-CAM105。

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