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首页> 外文期刊>Acta Biochimica Polonica >Expression of a constitutively active mutant of heat shock factor 1 under the control of testis-specific hst70 gene promoter in transgenic mice induces degeneration of seminiferous epithelium
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Expression of a constitutively active mutant of heat shock factor 1 under the control of testis-specific hst70 gene promoter in transgenic mice induces degeneration of seminiferous epithelium

机译:在睾丸特异性hst70基因启动子的控制下,热休克因子1的组成型活性突变体的表达在转基因小鼠中引起了生精上皮的变性

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摘要

Heat shock activates in somatic cells a set of genes encoding heat shock proteins which function as molecular chaperones. The basic mechanism by which these genes are activated is the interaction of the specific transcription factor HSF1 with a regulatory DNA sequence called heat shock element (HSE). In higher eukaryotes HSF1 is present in unstressed cells as inactive monomers which, in response to cellular stress, aggregate into transcriptionally competent homotrimers. In the present paper we showed that the expression of a transgene encoding mutated constitutively active HSF1 placed under the control of a spermatocyte-specific promoter derived from the hst70 gene severely affects spermatogenesis. We found the testes of transgenic mice to be significantly smaller than those of wild-type males and histological analysis showed massive degeneration of the seminiferous epithelium. The lumen of tubules was devoid of spermatids and spermatozoa and using the TUNEL method we demonstrated a high rate of spermatocyte apoptosis. The molecular mechanism by which constitutively active HSF1 arrest spermatogenesis is not known so far. One can assume that HSF1 can either induce or repress so far unknown target genes involved in germ cell apoptosis.
机译:热休克在体细胞中激活了一组编码热激蛋白质的基因,这些蛋白质起分子伴侣的作用。这些基因被激活的基本机制是特定转录因子HSF1与称为热休克元件(HSE)的调节性DNA序列的相互作用。在高等真核生物中,HSF1以无活性单体的形式存在于未受胁迫的细胞中,这些单体响应于细胞应激而聚集成转录上具有活性的三聚体。在本文中,我们显示了编码由hst70基因衍生的精子细胞特异性启动子控制的突变型组成型活性HSF1的转基因表达会严重影响精子发生。我们发现转基因小鼠的睾丸明显小于野生型雄性,组织学分析显示生精上皮细胞大量变性。肾小管的内腔没有精子和精子,使用TUNEL方法我们证明了精子细胞的凋亡率很高。迄今为止,尚不知道组成性活性HSF1阻止精子发生的分子机制。可以假设HSF1可以诱导或抑制到目前为止参与生殖细胞凋亡的未知靶基因。

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