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首页> 外文期刊>Fish & Shellfish Immunology >Isolation and characterization of homologous TRBP cDNA for RNA interference in Penaeus monodon.
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Isolation and characterization of homologous TRBP cDNA for RNA interference in Penaeus monodon.

机译:对虾斑节对虾RNA干扰的同源TRBP cDNA的分离与鉴定。

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摘要

The transactivation response RNA-binding protein (TRBP) interacts with Dicer and binds to double-stranded RNA as a critical component of the RNA-induced silencing complex, which is a key complex in the RNA interference pathway. The full-length cDNA of TRBP from the tiger prawn, Penaeus monodon, (PmTRBP; 1548 bp long with a 1029 bp coding region) was isolated. The encoded polypeptide of 343 amino acids had a predicted molecular mass of 36.8 kDa. Sequence homology and phylogenetic analysis indicated that PmTRBP was evolutionarily closest to TRBP1 from Litopenaeus vannamei, with the three double-stranded RNA-binding motifs that were typical of the TRBP family. Tissue expression profile analysis by quantitative real-time reverse transcription polymerase chain reaction showed that PmTRBP1 was constitutively expressed in all the examined tissues, with a predominant expression in the lymphatic organs and with the weakest expression in the ovaries. Significantly upregulated PmTRBP1 expression was elicited by systemic injections of Staphylococcus aureus, Vibrio vulnificus, and white spot syndrome virus, thereby revealing its pathogen inducibility. Furthermore, exogenous viral nucleoside analogs (high-molecular-weight poly(I:C) dsRNAs as well as R484 single-stranded RNA) were remarkably induced PmTRBP1 transcription at 48 h and 9 h post-injection, respectively, which suggested that PmTRBP1 might function in tiger prawn antibacterial and antiviral response.
机译:反式激活反应RNA结合蛋白(TRBP)与Dicer相互作用并与双链RNA结合,这是RNA诱导沉默复合物的关键成分,而沉默复合物是RNA干扰途径中的关键复合物。分离了虎虾对虾对虾TRBP的全长cDNA(PmTRBP;长1548 bp,编码区1029 bp)。编码的343个氨基酸的多肽的预测分子量为36.8 kDa。序列同源性和系统发育分析表明,PmTRBP在进化上最接近凡纳滨对虾TRBP1,具有三个TRBP家族典型的双链RNA结合基序。通过定量实时逆转录聚合酶链反应的组织表达谱分析表明,PmTRBP1在所有检查的组织中组成性表达,在淋巴器官中主要表达,在卵巢中最弱表达。系统性注射金黄色葡萄球菌,创伤弧菌和白斑综合症病毒引起PmTRBP1表达显着上调,从而揭示了其病原体诱导性。此外,外源病毒核苷类似物(高分子量聚(I:C)dsRNA以及R484单链RNA)分别在注射后48 h和9 h分别显着诱导了PmTRBP1转录,这表明PmTRBP1可能在虎虾的抗菌和抗病毒反应中起作用。

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