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发情周期中猪黄体血管内皮生长因子异构体及其受体的特征与差异表达

Characterization and differential expression of vascular endothelial growth factor isoforms and receptors in swine corpus luteum throughout estrous cycle.

作者信息

Ribeiro Luciana Andrea, Bacci Maria Laura, Seren Eraldo, Tamanini Carlo, Forni Monica

机构信息

Department of Morphophysiology and Animal Production, University of Bologna, (DIMORFIPA) Italy.

出版信息

Mol Reprod Dev. 2007 Feb;74(2):163-71. doi: 10.1002/mrd.20589.

DOI:10.1002/mrd.20589
PMID:16967516
Abstract

Corpus luteum (CL) undergoes growth and regression during each estrous cycle; these processes are accompanied by growth and regression of the luteal vascular bed. Vascular endothelial growth factor (VEGF) is the main regulator of angiogenesis, inducing endothelial cell proliferation, migration, vascular permeability, and vessel lumen formation. VEGF presents several isoforms that are produced by alternative splicing of the same mRNA transcript. We determined by real time RT-PCR the expression patterns of VEGF isoform and receptor mRNAs, as well as the VEGF protein levels in pig CL throughout a whole estrous cycle. Four novel VEGF isoforms (VEGF144, VEGF147, VEGF182, and VEGF164b) were found for the first time in swine and the seven identified isoforms can be grouped in four different patterns of expression. The most expressed splice variants were VEGF120 and VEGF164. All isoforms showed their highest mRNA levels in newly formed CLs (day 1), followed by a decrease during mid-late luteal phase (days 10-17), except for VEGF182, VEGF188 and VEGF144 that showed a differential regulation during late luteal phase (day 14) or at luteolysis (day 17). VEGF protein levels paralleled the most expressed and secreted VEGF120 and VEGF164 isoforms. The VEGF receptors mRNAs showed a different pattern of expression in relation to their ligands, increasing between day 1 and 3 and gradually decreasing during the mid-late luteal phase. The differential regulation of VEGF isoforms may suggest specific physiological roles for some of them, particularly in angioregression occurring during the apoptotic structural luteolysis.

摘要

黄体(CL)在每个发情周期中经历生长和退化;这些过程伴随着黄体血管床的生长和退化。血管内皮生长因子(VEGF)是血管生成的主要调节因子,可诱导内皮细胞增殖、迁移、血管通透性和血管腔形成。VEGF呈现出几种由同一mRNA转录本的可变剪接产生的异构体。我们通过实时RT-PCR确定了整个发情周期中猪黄体中VEGF异构体和受体mRNA的表达模式以及VEGF蛋白水平。首次在猪中发现了四种新的VEGF异构体(VEGF144、VEGF147、VEGF182和VEGF164b),所鉴定的七种异构体可分为四种不同的表达模式。表达最多的剪接变体是VEGF120和VEGF164。所有异构体在新形成的黄体(第1天)中显示出最高的mRNA水平,随后在黄体中期至后期(第10 - 17天)下降,但VEGF182、VEGF188和VEGF144在黄体后期(第14天)或黄体溶解期(第17天)表现出不同的调节。VEGF蛋白水平与表达和分泌最多的VEGF120和VEGF164异构体平行。VEGF受体mRNA与其配体相比显示出不同的表达模式,在第1天至第3天增加,在黄体中期至后期逐渐下降。VEGF异构体的差异调节可能表明其中一些具有特定的生理作用,特别是在凋亡性结构黄体溶解过程中发生的血管消退中。

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