首页> 外文期刊>Insect Molecular Biology >Robust heat-inducible gene expression by two endogenous hsp70-derived promoters in transgenic Aedes aegypti.
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Robust heat-inducible gene expression by two endogenous hsp70-derived promoters in transgenic Aedes aegypti.

机译:两个内源性 hsp70 启动子在转基因伊蚊中的稳健的热诱导基因表达。

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摘要

Aedes aegypti is an important vector of the viruses that cause dengue fever, dengue haemorrhagic fever and yellow fever. Reverse genetic approaches to the study of gene function in this mosquito have been limited by the lack of a robust inducible promoter to allow precise temporal control over a protein-encoding or hairpin RNA transgene. Likewise, investigations into the molecular and biochemical basis of vector competence would benefit from the ability to activate an antipathogen molecule at specific times during infection. We have characterized the ability of genomic sequences derived from two Ae. aegypti heat shock protein 70 (hsp70) genes to drive heat-inducible expression of a reporter in both transient and germline transformation contexts. AaHsp70-luciferase transcripts accumulated specifically after heat shock, and displayed a pattern of rapid induction and decay similar to endogenous AaHsp70 genes. Luciferase expression in transgenic Ae. aegypti increased by ~25-50-fold in whole adults by 4 h after heat-shock, with significant activity (~20-fold) remaining at 24h. Heat-induced expression was even more dramatic in midgut tissues, with one strain showing a ~2500-fold increase in luciferase activity. The AaHsp70 promoters described could be valuable for gene function studies as well as for the precise timing of the expression of antipathogen molecules.
机译:埃及伊蚊是引起登革热,登革出血热和黄热病的重要病毒载体。研究这种蚊子中的基因功能的反向遗传学方法由于缺少强大的诱导型启动子而无法对蛋白编码或发夹RNA转基因进行精确的时间控制,因此受到了限制。同样,对载体能力的分子和生化基础的研究将受益于在感染过程中特定时间激活抗病原体分子的能力。我们已经表征了衍生自两个Ae的基因组序列的能力。埃及热休克蛋白70 hsp70 )基因可在瞬时和种系转化环境中驱动报告基因的热诱导表达。 AaHsp70 -荧光素酶转录物在热休克后特别积累,并显示出与内源性 AaHsp70 基因相似的快速诱导和衰变模式。荧光素酶在转基因Ae中的表达。在热休克后的4小时内,整个成年人的埃及伊蚊增加了约25至50倍,而在24小时内仍保留了明显的活性(约20倍)。热诱导的表达在中肠组织中更为显着,一种菌株显示萤光素酶活性增加了约2500倍。所述的 AaHsp70 启动子对于基因功能研究以及抗病原体分子表达的精确时间可能是有价值的。

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