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首页> 外文期刊>Journal of Shellfish Research >AN INHIBITOR kappa B HOMOLOG FROM THE BIVALVE MOLLUSC SOLEN GRANDIS THAT RESPONDS TO IMMUNE CHALLENGE
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AN INHIBITOR kappa B HOMOLOG FROM THE BIVALVE MOLLUSC SOLEN GRANDIS THAT RESPONDS TO IMMUNE CHALLENGE

机译:来自双壳软体动物SORAND GRANDIS的抑制剂kappa B同源物,可应对免疫挑战

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The nuclear factor-kappa B (NF-kappa B) signaling pathway has been studied extensively in mammalians and insects but has been less well investigated in marine molluscs. Inhibitor of kappa B (I kappa B), an important component of the NF-kappa B signaling pathway, serves as a crucial mediator of the innate immune system. A homolog of I kappa B was identified in a razor clam (Solen grandis), designated as SgI kappa B, and its messenger RNA expression was detected both in tissues and towards pathogen-associated molecular patterns. Full-length complementary DNA of SgI kappa B is 2,232 bp, containing a 181-bp 5' untranslated region (UTR) and a 970-bp 3' UTR with a poly (A) tail. The open reading frame is 1,080 bp, encoding a 359-amino acid polypeptide with a predicted molecular weight of 40.1 kDa and an isoelectric point of 4.88. A potential PEST motif (E2SNDLEMDTCPLEMDS17) and the I kappa B degradation motif (ES(44)GYKS(48)) are located at the N-terminus, and 2 conserved casein kinase II phosphorylation sites (S337DEE340 and S346YDD349) exist at the C terminus. The presence of 6 conserved ankyrin repeats in SgI kappa B and its close phylogenetic relationship with other I kappa Bs strongly suggest that SgIkB belongs to the I kappa B superfamily. Messenger RNA of SgI kappa B is expressed constitutively in various tissues of healthy S. grandis, with the greatest expression in gill and hepatopancreas, followed by gonad, mantle, hemocyte, and muscle in descending order. Messenger RNA expression of SgI kappa B in hemocytes is upregulated significantly to varying degrees (P 0.01) on stimulation with lipopolysaccharide, peptidoglycan, and beta-1,3-glucan. The results indicate the existence of a NF-kappa B signaling pathway in S. grandis and provide evidence for possible regulatory mechanisms during an immune challenge.
机译:核因子-κB(NF-κB)信号通路已在哺乳动物和昆虫中进行了广泛研究,但在海洋软体动物中的研究较少。 NF-κB信号传导通路的重要组成部分-κB(I kappa B)抑制剂是先天免疫系统的重要介质。在剃刀蛤(Solen grandis)中鉴定出IκB的同系物,命名为SgIκB,并且在组织中以及与病原体相关的分子模式中均检测到其信使RNA表达。 SgI kappa B的全长互补DNA为2232 bp,包含181 bp的5'非翻译区(UTR)和970 bp的3'UTR,带有聚(A)尾巴。开放阅读框为1,080 bp,编码359个氨基酸的多肽,预测分子量为40.1 kDa,等电点为4.88。潜在的PEST基序(E2SNDLEMDTCPLEMDS17)和IκB降解基序(ES(44)GYKS(48))位于N端,C端存在2个保守的酪蛋白激酶II磷酸化位点(S337DEE340和S346YDD349)。 。 SgIκB中6个保守的锚蛋白重复序列​​的存在及其与其他IκB的密切系统发育关系强烈表明SgIkB属于IκB超家族。 SgIκB的信使RNA在健康的葡萄球菌的各种组织中组成性表达,在g和肝胰腺中表达最多,其次是性腺,地幔,血细胞和肌肉,其降序排列。脂多糖,肽聚糖和β-1,3-葡聚糖刺激后,血细胞中SgIκB的Messenger RNA表达显着上调至不同程度(P <0.01)。结果表明在大链球菌中存在NF-κB信号通路,并为免疫攻击过程中可能的调控机制提供了证据。

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