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从虎纹蛙中鉴定出一种胰高血糖素原cDNA,其编码两种胰高血糖素样肽-1(GLP-1),并以组织特异性方式进行可变剪接。

Identification of a proglucagon cDNA from Rana tigrina rugulosa that encodes two GLP-1s and that is alternatively spliced in a tissue-specific manner.

作者信息

Yeung C M, Chow B K

机构信息

Department of Zoology, University of Hong Kong, Pokfulam Road, Hong Kong.

出版信息

Gen Comp Endocrinol. 2001 Nov;124(2):144-51. doi: 10.1006/gcen.2001.7697.

Abstract

Glucagon plays a pivotal role in the regulation of metabolism. A glucagon receptor has been previously characterized in the frog, Rana tigrina rugulosa, and the frog and human glucagon receptors have been shown to possess similar binding affinities toward human glucagon. To study the structural evolution of glucagon peptide and its receptor in vertebrates, in the current study, a proglucagon cDNA from the same frog species was cloned. Interestingly, in contrast to the mammalian proglucagons that contain only one GLP-1 peptide, the frog proglucagon cDNA encodes two GLP-1 peptides (GLP-1A and GLP-1B) in addition to a glucagon peptide and a glucagon-like peptide 2 (GLP-2). By reverse transcriptase-PCR (RT-PCR) analysis, the proglucagon gene expression was widely detected in the brain, colon, small intestine, liver, lung, and pancreas, suggesting that the proglucagon-derived peptides have diverse functions in frogs. Moreover, tissue-specific alternative mRNA splicing was observed in the brain, colon, and pancreas. In these tissues, proglucagon transcripts with a 135 bp in frame deletion encoding GLP-1A were found. This splicing event in R. tigrina rugulosa is novel because it deletes a GLP-1 encoding sequence instead of the GLP-2 observed in other vertebrates. These findings should enhance understanding of the proglucagon evolution, structure, and expression in vertebrates.

摘要

胰高血糖素在新陈代谢的调节中起着关键作用。先前已在虎纹蛙中鉴定出胰高血糖素受体,并且已证明蛙和人胰高血糖素受体对人胰高血糖素具有相似的结合亲和力。为了研究脊椎动物中胰高血糖素肽及其受体的结构进化,在本研究中,克隆了来自同一蛙种的胰高血糖素原cDNA。有趣的是,与仅包含一种GLP-1肽的哺乳动物胰高血糖素原不同,蛙胰高血糖素原cDNA除了编码一种胰高血糖素肽和一种胰高血糖素样肽2(GLP-2)外,还编码两种GLP-1肽(GLP-1A和GLP-1B)。通过逆转录酶PCR(RT-PCR)分析,在脑、结肠、小肠、肝脏、肺和胰腺中广泛检测到胰高血糖素原基因表达,这表明胰高血糖素原衍生的肽在蛙中具有多种功能。此外,在脑、结肠和胰腺中观察到组织特异性的可变mRNA剪接。在这些组织中,发现了编码GLP-1A的有135 bp框内缺失的胰高血糖素原转录本。虎纹蛙中的这种剪接事件是新颖的,因为它删除了一个GLP-1编码序列,而不是在其他脊椎动物中观察到的GLP-2。这些发现应能增强对脊椎动物中胰高血糖素原进化、结构和表达的理解。

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