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首页> 外文期刊>Veterinary research >Molecular cloning and characterization of a novel peptidase from Trichinella spiralis and protective immunity elicited by the peptidase in BALB/c mice
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Molecular cloning and characterization of a novel peptidase from Trichinella spiralis and protective immunity elicited by the peptidase in BALB/c mice

机译:Palb / C小鼠肽酶引出的Trichinella spirlisis和保护免疫的分子克隆与表征

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In our previous studies, a novel T. spiralis peptidase (TsP) was identified among the excretory/secretory (ES) proteins of T. spiralis intestinal infective larvae (IIL) and T. spiralis at the adult worm (AW) stage using immunoproteomics, but the biological function of TsP in the life cycle of T. spiralis is not clear. The objective of this study was to investigate the biological properties and functions of TsP in larval intrusion and protective immunity induced by immunization with rTsP. The complete TsP cDNA sequence was cloned and expressed. The results of RT-PCR, indirect immunofluorescence assay (IIFA) and western blotting revealed that TsP is a surface and secretory protein expressed in T. spiralis at different stages (muscle larvae, IIL, AWs and newborn larvae) that is principally localized at the epicuticle of the nematode. rTsP facilitated the larval intrusion of intestinal epithelial cells (IECs) and intestinal mucosa, whereas anti-rTsP antibodies suppressed larval intrusion; these facilitative and suppressive roles were dose-dependently related to rTsP or anti-rTsP antibodies. Immunization of mice with rTsP triggered an obvious humoral immune response (high levels of IgG, IgG1/IgG2a, and sIgA) and also elicited systemic (spleen) and intestinal local mucosal (mesenteric lymph node) cellular immune responses, as demonstrated by an evident increase in the cytokines IFN-γ and IL-4. Immunization of mice with rTsP reduced the numbers of intestinal adult worms by 38.6% and muscle larvae by 41.93%. These results demonstrate that TsP plays a vital role in the intrusion, development and survival of T. spiralis in hosts and is a promising candidate target molecule for anti-Trichinella vaccines.
机译:在我们以前的研究中,在使用免疫蛋白质组织的成人蠕虫(AW)阶段的T. spiralis肠道感染幼虫(IIL)和T. spiralis的排泄/分泌蛋白质中鉴定了一种新的T.螺肽酶(TSP)。但TSP在T. Spiralis生命周期中的生物学功能尚不清楚。本研究的目的是探讨TSP在幼虫侵入和通过RTSP免疫诱导的保护免疫中的生物学特性和功能。完全TSP cDNA序列被克隆并表达。 RT-PCR,间接免疫荧光测定(IIFA)和Western印迹的结果显示,TSP是在不同阶段(肌肉幼虫,IIL,AWS和新生儿幼虫)的T.Taplalis中表达的表面和分泌蛋白。主要是本地化的线虫的脱毛症。 RTSP促进了肠上皮细胞(IECS)和肠粘膜的幼虫侵入,而抗RTSP抗体抑制了幼虫侵入;这些促进和抑制作用与RTSP或抗RTSP抗体依赖性依赖性。用RTSP免疫小鼠引发了明显的体液免疫应答(高水平的IgG,IgG1 / IgG2A和SIGA),并且还引发了全身(脾)和肠道局部粘膜(肠系膜淋巴结)细胞免疫反应,如明显的增加所证明在细胞因子IFN-γ和IL-4中。用RTSP免疫小鼠将肠道成人蠕虫的数量减少38.6%,肌肉幼虫减少41.93%。这些结果表明,TSP在宿主中T.Spiralis的入侵,开发和存活方面发挥着至关重要的作用,并且是抗Trichinella疫苗的有希望的候选目标分子。

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