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A dominant-negative isoform of hypoxia-inducible factor-1 alpha specifically expressed in human testis.

机译:低氧诱导因子-1α的显性负同种型在人类睾丸中特异性表达。

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摘要

Spermatogenesis in the seminiferous tubuli of the testis occurs under a high proliferation rate, suggesting considerable oxygen consumption. Because of the lack of blood vessels, the oxygen partial pressure in the lumen of these tubuli is very low. We previously identified a testis isoform of the hypoxia-inducible factor (HIF)-1alpha in the mouse, termed mHIF-1alphaI.1. Here, we demonstrate that expression of mHIF-1alphaI.1 increases during puberty, further demonstrating its gene induction in postmeiotic germ cells. Using 5'-rapid amplification of cDNA ends, we identified a novel HIF-1alpha isoform in the human testis, called hHIF-1alphaTe. Like mHIF-1alphaI.1, hHIF-1alphaTe mRNA is derived from an alternative promoter-first exon combination, but with a different genomic organization and a different nucleotide sequence. Reverse transcription-polymerase chain reaction analysis confirmed that hHIF-1alphaTe is exclusively expressed in the testis. As determined by immunofluorescence of ejaculated sperm cells, HIF-1alpha protein is mainly localized in the postacrosomal head and in the midpiece of spermatozoa. Though overlapping with mitochondrial localization in human and mouse spermatozoa, neither hHIF-1alphaTe nor hHIF-1alpha associated with mitochondria. In contrast with the ubiquitously expressed HIF-1alpha protein and the mouse testis-specific mHIF-1alphaI.1 isoform, the hHIF-1alphaTe mRNA sequence predicts a protein with an N-terminal truncation of the DNA-binding domain. As shown by yeast two-hybrid assays, hHIF-1alphaTe still formed heterodimeric complexes with HIF-1beta. However, hHIF-1alphaTe was incapable of forming a DNA-binding HIF-1 complex. Overexpression of exogenous hHIF-1alphaTe resulted in the inhibition of the endogenous HIF-1 transcriptional activity, demonstrating that the testis-specific hHIF-1alphaTe isoform is a dominant-negative regulator of normal HIF-1 activity.
机译:睾丸生精小管中的精子发生在高增殖率下发生,表明耗氧量很大。由于缺乏血管,这些小管腔内的氧气分压非常低。我们先前在小鼠中发现了缺氧诱导因子(HIF)-1alpha的睾丸亚型,称为mHIF-1alphaI.1。在这里,我们证明了在青春期mHIF-1alphaI.1的表达增加,进一步证明了减数分裂后生殖细胞中其基因的诱导。使用cDNA末端的5'-快速扩增,我们在人的睾丸中鉴定出一种新型的HIF-1alpha亚型,称为hHIF-1alphaTe。像mHIF-1alphaI.1一样,hHIF-1alphaTe mRNA衍生自另一个启动子-第一个外显子组合,但具有不同的基因组组织和不同的核苷酸序列。逆转录聚合酶链反应分析证实hHIF-1alphaTe仅在睾丸中表达。通过射精细胞的免疫荧光测定,HIF-1α蛋白主要位于精子后头和中段。尽管与人类和小鼠精子中的线粒体定位重叠,但hHIF-1alphaTe和hHIF-1alpha均与线粒体无关。与普遍表达的HIF-1alpha蛋白和小鼠睾丸特异的mHIF-1alphaI.1亚型相反,hHIF-1alphaTe mRNA序列预测该蛋白具有DNA结合结构域的N端截短。如酵母双杂交试验所示,hHIF-1alphaTe仍与HIF-1beta形成异二聚体复合物。但是,hHIF-1alphaTe无法形成结合DNA的HIF-1复合物。外源hHIF-1alphaTe的过表达导致内源HIF-1转录活性的抑制,表明睾丸特异性hHIF-1alphaTe同工型是正常HIF-1活性的显性负调节剂。

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