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人神经内分泌肿瘤中胰岛素样生长因子1受体可变剪接mRNA形式的差异表达

Differential expression of alternatively spliced mRNA forms of the insulin-like growth factor 1 receptor in human neuroendocrine tumors.

作者信息

Vitale Lorenza, Lenzi Luca, Huntsman Shane A, Canaider Silvia, Frabetti Flavia, Casadei Raffaella, Facchin Federica, Carinci Paolo, Zannotti Maria, Coppola Domenico, Strippoli Pierluigi

机构信息

Dipartimento di Istologia, Embriologia e Biologia Applicata, Università di Bologna, I-40126 Bologna, Italy.

出版信息

Oncol Rep. 2006 May;15(5):1249-56.

Abstract

The activation of the insulin-like growth factor 1/IGF1 receptor system (IGF1/IGF1R) is a critical event in the transformation and tumorigenicity processes in a wide variety of human tumors. The IGF1/IGF1R system has been recently studied in carcinoid tumors that often arise in the gastrointestinal tract; these tumors are characterized by hypersecretion of bioamines and neuropeptides, leading to functional tumor disease. Two alternatively spliced IGF1R mRNA transcripts have been described to differ by only three nucleotides (CAG) in the coding sequence, resulting in an amino-acid change from the originally described Thr-Gly to an Arg in the extracellular portion of the receptor beta subunit. In transfected Chinese hamster ovary cells, the form without CAG (CAG-) exhibited an approximate 2-fold increase in IGF1 stimulation of activities required for its mitogenic properties. In this study, we examine the relative expression of the two IGF1R mRNA isoforms by a semiquantitative RT-PCR approach using highly standardized conditions, beta-2 microglobulin (B2M) as a reference gene and gel imaging analysis. We analyzed a large series of human neuroendocrine tumors (32 samples) and 9 normal tissues. A significant higher expression of both isoforms in the tumor samples (approximately 2-fold increase) was found, while a constant CAG+/CAG- IGF1R mRNA isoforms of an approximate 3:1 ratio was observed in all tumoral and normal cell types studied. The phylogenetic study of the IGF1R locus in several species suggests that human IGF1R CAG- mRNA isoform is evolutionarily more recent compared to the IGF1R CAG+ mRNA isoform and it could be used by the splicing apparatus at this intron/exon junction with a lower efficiency. This study highlights the relevance of IGF1R mRNA expression in neuroendocrine tumor cells, and the constant presence of 'subtle' alternative splicing for the IGF1R locus.

摘要

胰岛素样生长因子1/IGF1受体系统(IGF1/IGF1R)的激活是多种人类肿瘤发生转化和致瘤过程中的关键事件。最近,IGF1/IGF1R系统已在常发生于胃肠道的类癌肿瘤中得到研究;这些肿瘤的特征是生物胺和神经肽分泌过多,导致功能性肿瘤疾病。已描述了两种选择性剪接的IGF1R mRNA转录本,它们在编码序列中仅相差三个核苷酸(CAG),导致受体β亚基细胞外部分的氨基酸从最初描述的苏氨酸-甘氨酸变为精氨酸。在转染的中国仓鼠卵巢细胞中,没有CAG的形式(CAG-)在IGF1刺激其促有丝分裂特性所需的活性方面表现出约2倍的增加。在本研究中,我们使用高度标准化的条件、β-2微球蛋白(B2M)作为参考基因并通过凝胶成像分析,采用半定量RT-PCR方法检测两种IGF1R mRNA亚型的相对表达。我们分析了大量人类神经内分泌肿瘤(32个样本)和9个正常组织。发现肿瘤样本中两种亚型的表达均显著更高(约增加2倍),而在所研究的所有肿瘤和正常细胞类型中均观察到CAG+/CAG- IGF1R mRNA亚型的恒定比例约为3:1。对几种物种中IGF1R基因座的系统发育研究表明,与IGF1R CAG+ mRNA亚型相比,人类IGF1R CAG- mRNA亚型在进化上更新近,并且剪接装置在这个内含子/外显子连接处使用它的效率较低。这项研究突出了IGF1R mRNA表达在神经内分泌肿瘤细胞中的相关性,以及IGF1R基因座持续存在的“细微”选择性剪接。

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