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Molecular characterization of an adiponectin receptor homolog in the white leg shrimp Litopenaeus vannamei

机译:白腿虾对虾凡纳滨对虾中脂联素受体同源物的分子表征

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摘要

Adiponectin (AdipoQ) and its receptors (AdipoRs) are strongly related to growth and development of skeletal muscle, as well as glucose and lipid metabolism in vertebrates. Herein we report the identification of the first full-length cDNA encoding an AdipoR homolog (Liv-AdipoR) from the decapod crustacean Litopenaeus vannamei using a combination of next generation sequencing (NGS) technology and bioinformatics analysis. The full-length Liv-AdipoR (1,245 bp) encoded a protein that exhibited the canonical seven transmembrane domains (7TMs) and the inversed topology that characterize members of the progestin and adipoQ receptor (PAQR) family. Based on the obtained sequence information, only a single orthologous AdipoR gene appears to exist in arthropods, whereas two paralogs, AdipoR1 and AdipoR2, have evolved in vertebrates. Transcriptional analysis suggested that the single Liv-AdipoR gene appears to serve the functions of two mammalian AdipoRs. At 72 h after injection of 50 pmol Liv-AdipoR dsRNA (340 bp) into L. vannamei thoracic muscle and deep abdominal muscle, transcription levels of Liv-AdipoR decreased by 93% and 97%, respectively. This confirmed optimal conditions for RNAi of Liv-AdipoR. Knockdown of Liv-AdipoR resulted in significant changes in the plasma levels of ammonia, 3-methylhistine, and ornithine, but not plasma glucose, suggesting that that Liv-AdipoR is important for maintaining muscle fibers. The chronic effect of Liv-AdipoR dsRNA injection was increased mortality. Transcriptomic analysis showed that 804 contigs were upregulated and 212 contigs were downregulated by the knockdown of Liv-AdipoR in deep abdominal muscle. The significantly upregulated genes were categorized as four main functional groups: RNA-editing and transcriptional regulators, molecular chaperones, metabolic regulators, and channel proteins.
机译:脂联素(AdipoQ)及其受体(AdipoRs)与脊椎动物骨骼肌的生长和发育以及葡萄糖和脂质代谢密切相关。本文中,我们报告了使用下一代测序(NGS)技术和生物信息学分析相结合的方法,从头足类甲壳动物对虾凡纳滨对虾(Litopenaeus vannamei)中编码AdipoR同源物(Liv-AdipoR)的第一个全长cDNA的鉴定。全长Liv-AdipoR(1,245 bp)编码一种蛋白质,该蛋白质具有典型的七个跨膜结构域(7TM)和逆向拓扑结构,该结构表征孕激素和adipoQ受体(PAQR)家族的成员。根据获得的序列信息,节肢动物中似乎仅存在一个直系同源AdipoR基因,而脊椎动物中已进化出两个旁系同源物AdipoR1和AdipoR2。转录分析表明,单个Liv-AdipoR基因似乎具有两个哺乳动物AdipoR的功能。在向南美白对虾胸肌和深腹肌注射50 pmol Liv-AdipoR dsRNA(340 bp)后的72小时,Liv-AdipoR的转录水平分别降低了93%和97%。这证实了Liv-AdipoR RNAi的最佳条件。敲除Liv-AdipoR会导致血浆氨,3-甲基组氨酸和鸟氨酸的水平发生重大变化,但血浆葡萄糖却无变化,这表明Liv-AdipoR对维持肌肉纤维很重要。 Liv-AdipoR dsRNA注射的慢性影响是增加死亡率。转录组分析显示,通过深腹肌Liv-AdipoR的敲低,上调804个重叠群,下调212个重叠群。显着上调的基因分为四个主要功能组:RNA编辑和转录调节因子,分子伴侣,代谢调节因子和通道蛋白。

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