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协调人肝肿瘤中纤连蛋白前体信使核糖核酸在ED - A、ED - B和CS1区域的可变剪接的共发育调控。

Coordinate oncodevelopmental modulation of alternative splicing of fibronectin pre-messenger RNA at ED-A, ED-B, and CS1 regions in human liver tumors.

作者信息

Oyama F, Hirohashi S, Sakamoto M, Titani K, Sekiguchi K

机构信息

Institute for Comprehensive Medical Science, Fujita Health University, Aichi, Japan.

出版信息

Cancer Res. 1993 May 1;53(9):2005-11.

PMID:8481903
Abstract

The molecular diversity of fibronectin arises from alternative RNA splicing at regions termed ED-A, ED-B, and IIICS. We investigated the splicing patterns of fibronectin pre-mRNA at both ED-B and IIICS regions in various human liver tissues with an emphasis on the expression of the alternative cell adhesive site CS1 within the IIICS region. The relative abundance of the fibronectin mRNA containing the CS1 sequence was significantly increased in both fetal and cancerous liver tissues, although it was not affected in nonmalignant tissues with chronic hepatitis and cirrhosis. Similarly, the relative abundance of the fibronectin mRNA containing the ED-B region was also increased in both fetal liver and liver tumors, showing a close parallelism with the splicing pattern at the ED-A region. Immunohistochemical examination of cancerous liver tissues with monoclonal antibodies directed to the ED-A and ED-B segments revealed that the fibronectin isoforms containing these extra peptide segments were specifically deposited in the tumor nodules. Other genes encoding kininogen, gamma chain of fibrinogen, and beta-amyloid protein precursor, all of which had been shown to be alternatively processed, did not show any significant alteration in the splicing pattern in cancerous liver tissues. These results indicate that the alternative splicing of fibronectin pre-mRNA at the ED-A, ED-B, and IIICS regions is coordinately modulated in both fetal and cancerous liver tissues toward inclusion of the extra peptide segments and that not all but only selected genes are susceptible for "fine tuning" of alternative RNA splicing in cancerous liver tissues.

摘要

纤连蛋白的分子多样性源于在称为ED-A、ED-B和IIICS区域的可变RNA剪接。我们研究了各种人类肝脏组织中纤连蛋白前体mRNA在ED-B和IIICS区域的剪接模式,重点关注IIICS区域内可变细胞粘附位点CS1的表达。含有CS1序列的纤连蛋白mRNA的相对丰度在胎儿肝脏组织和癌组织中均显著增加,尽管在慢性肝炎和肝硬化的非恶性组织中未受影响。同样,含有ED-B区域的纤连蛋白mRNA的相对丰度在胎儿肝脏和肝脏肿瘤中也增加,与ED-A区域的剪接模式呈现密切的平行关系。用针对ED-A和ED-B片段的单克隆抗体对癌组织进行免疫组织化学检查发现,含有这些额外肽段的纤连蛋白异构体特异性沉积在肿瘤结节中。其他编码激肽原、纤维蛋白原γ链和β-淀粉样蛋白前体的基因,所有这些基因均已显示存在可变加工,但在癌组织中的剪接模式未显示任何显著改变。这些结果表明,在胎儿肝脏组织和癌组织中,纤连蛋白前体mRNA在ED-A、ED-B和IIICS区域的可变剪接朝着包含额外肽段的方向受到协同调节,并且在癌组织中并非所有基因,而是只有选定的基因易于进行可变RNA剪接的“微调”。

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