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首页> 外文期刊>American Journal of Pathology: Official Publication of the American Association of Pathologists >Alternative splicing of pre-mRNA in cancer: focus on G protein-coupled peptide hormone receptors.
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Alternative splicing of pre-mRNA in cancer: focus on G protein-coupled peptide hormone receptors.

机译:前mRNA在癌症中的选择性剪接:专注于G蛋白偶联肽激素受体。

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Through alternative splicing, multiple different transcripts can be generated from a single gene. Alternative splicing represents an important molecular mechanism of gene regulation in physiological processes such as developmental programming as well as in disease. In cancer, splicing is significantly altered. Tumors express a different collection of alternative spliceoforms than normal tissues. Many tumor-associated splice variants arise from genes with an established role in carcinogenesis or tumor progression, and their functions can be oncogenic. This raises the possibility that products of alternative splicing play a pathogenic role in cancer. Moreover, cancer-associated spliceoforms represent potential diagnostic biomarkers and therapeutic targets. G protein-coupled peptide hormone receptors provide a good illustration of alternative splicing in cancer. The wild-type forms of these receptors have long been known to be expressed in cancer and to modulate tumor cell functions. They are also recognized as attractive clinical targets. Recently, splice variants of these receptors have been increasingly identified in various types of cancer. In particular, alternative cholecystokinin type 2, secretin, and growth hormone-releasing hormone receptor spliceoforms are expressed in tumors. Peptide hormone receptor splice variants can fundamentally differ from their wild-type receptor counterparts in pharmacological and functional characteristics, in their distribution in normal and malignant tissues, and in their potential use for clinical applications.
机译:通过选择性剪接,可以从单个基因产生多个不同的转录本。选择性剪接代表诸如发育程序设计以及疾病中的生理过程中基因调节的重要分子机制。在癌症中,剪接显着改变。肿瘤表达的替代剪接形式与正常组织不同。许多与肿瘤相关的剪接变体来自在致癌或肿瘤进展中具有确定作用的基因,它们的功能可能是致癌的。这增加了选择性剪接产物在癌症中发挥致病作用的可能性。此外,癌症相关的剪接形式代表潜在的诊断生物标志物和治疗目标。 G蛋白偶联的肽激素受体为癌症中的选择性剪接提供了很好的例证。早就知道这些受体的野生型形式在癌症中表达并调节肿瘤细胞的功能。它们也被认为是有吸引力的临床靶标。最近,在各种类型的癌症中越来越多地鉴定出这些受体的剪接变体。特别是,在肿瘤中表达了2型胆囊收缩素,促胰液素和生长激素释放激素受体剪接形式。肽激素受体剪接变体在药理和功能特性,它们在正常和恶性组织中的分布以及在临床上的潜在用途方面可以与野生型受体对应物根本不同。

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