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旋毛虫金属蛋白酶 Tsdpy31 参与幼虫蜕皮和发育。

A metalloproteinase Tsdpy31 from Trichinella spiralis participates in larval molting and development.

机构信息

Department of Parasitology, Medical College, Zhengzhou University, Zhengzhou 450052, PR China.

Department of Parasitology, Medical College, Zhengzhou University, Zhengzhou 450052, PR China.

出版信息

Int J Biol Macromol. 2021 Dec 1;192:883-894. doi: 10.1016/j.ijbiomac.2021.10.021. Epub 2021 Oct 14.

Abstract

Trichinellosis is a serious food-borne zoonotic parasitic disease with global distribution, causing serious harm to public health and food safety. Molting is prerequisite for intestinal larval development in the life cycle of T. spiralis. Metalloproteinases play an important role in the molting process of T. spiralis intestinal infective larvae (IIL). In this study, the metalloproteinase Tsdpy31 was cloned, expressed and characterized. The results revealed that the Tsdpy31 was expressed at various T. spiralis stages and it was principally located in cuticle, hypodermis and embryos of the nematode. Recombinant Tsdpy31 (rTsdpy31) had the catalytic activity of natural metalloproteinase. Silencing of Tsdpy31 increased the permeability of larval new cuticle. When the mice were orally challenged with dsRNA treated- muscle larvae, the burden of intestinal adult and muscle larvae in Tsdpy31 dsRNA treatment group was significantly reduced, compared with the control green fluorescent protein (GFP) dsRNA and PBS groups (P < 0.05). Tsdpy31 may play a major role in the new cuticle synthesis and old cuticle shedding. Tsdpy31 also participates in T. spiralis embryonic development. We conclude that Tsdpy31 could be a candidate vaccine target molecule against intestinal T. spiralis ecdysis and development.

摘要

旋毛虫病是一种具有全球分布的严重食源性人畜共患寄生虫病,对公共卫生和食品安全造成严重危害。蜕皮是旋毛虫生活史中肠道幼虫发育的前提。金属蛋白酶在旋毛虫肠道感染性幼虫(IIL)的蜕皮过程中发挥重要作用。在这项研究中,克隆、表达和表征了金属蛋白酶 Tsdpy31。结果表明,Tsdpy31 在旋毛虫的各个阶段都有表达,主要位于线虫的角质层、皮下组织和胚胎中。重组 Tsdpy31(rTsdpy31)具有天然金属蛋白酶的催化活性。Tsdpy31 的沉默增加了幼虫新角质层的通透性。当用 dsRNA 处理的肌幼虫对小鼠进行口服攻毒时,与对照绿色荧光蛋白(GFP)dsRNA 和 PBS 组相比,Tsdpy31 dsRNA 处理组肠道成虫和肌肉幼虫的负荷明显降低(P < 0.05)。Tsdpy31 可能在新角质层合成和旧角质层脱落中起主要作用。Tsdpy31 还参与旋毛虫胚胎发育。我们得出结论,Tsdpy31 可能是一种针对肠道旋毛虫蜕皮和发育的候选疫苗靶分子。

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