College of Veterinary Medicine, Nanjing Agricultural University, Nanjing, People's Republic of China.
Parasit Vectors. 2017 Sep 18;10(1):425. doi: 10.1186/s13071-017-2368-1.
Haemonchosis is a disease of the small ruminant caused by a nematode parasite Haemonchus contortus, and it is most important and alarming challenges to the small ruminant's production. The infection of the H. contortus could cause high economic losses worldwide. H. contortus is a blood feeding parasite which penetrates into the abomasal mucosa to feed the blood of the host and causing the anemia and decreased total plasma protein. Modulation and suppression of the immune response of the host by nematode parasites have been reported extensively, and the cysteine protease inhibitor (cystatin) is identified as one of the major immunomodulators.
The recombinant protein of HCcyst-3 was expressed in a histidine-tagged fusion soluble form in Escherichia coli, and its inhibitory activity against cathepsin L, B, as well as papain, were identified by fluorogenic substrate analysis. Native HCcyst-3 protein was localized by an Immunohistochemical test. The immunomodulatory effects of HCcyst-3 on cytokine secretion, MHC molecule expression, NO production and phagocytosis were observed by co-incubation of rHCcyst-3 with goat monocytes.
We cloned and produced recombinant cystatin protein from H. contortus (rHCcyst-3) and investigated its immunomodulatory effects on goat monocyte. The rHCcyst-3 protein is biologically functional as shown by its ability to inhibit the protease activity of cathepsin L, cathepsin B, and papain. The immunohistochemical test demonstrated that the native HCcyst-3 protein was predominantly localized at the body surface and internal surface of the worm's gut. We demonstrated that rHCcyst-3 could be distinguished by antisera from goat experimentally infected with H. contortus and could uptake by goat monocytes. The results showed that the engagement of rHCcyst-3 decreased the production of TNF-α, IL-1β and IL-12p40. However, it significantly increased the secretion of IL-10 and TGF-β1 in goat monocytes. After rHCcyst-3 exposure, the expression of MHC-II on goat monocytes was restricted. Moreover, rHCcyst-3 could upregulate LPS induced NO production of goat monocytes. Phagocytotic assay by FITC-dextran internalization showed that rHCcyst-3 inhibited the phagocytosis of goat monocytes.
Our results suggested that the recombinant cystatin from H. contortus (rHCcyst-3) significantly modulated goat monocyte function in multiple aspects.
血矛线虫病是一种由寄生线虫血矛线虫引起的小反刍动物疾病,是小反刍动物生产中最重要和最令人担忧的挑战。该线虫的感染会在全球范围内造成巨大的经济损失。血矛线虫是一种以血液为食的寄生虫,它穿透皱胃黏膜以吸食宿主的血液,导致贫血和总血浆蛋白减少。广泛报道了线虫寄生虫对宿主免疫反应的调节和抑制,半胱氨酸蛋白酶抑制剂(cystatin)被确定为主要免疫调节剂之一。
在大肠杆菌中以组氨酸标记融合可溶性形式表达重组蛋白 HCcyst-3,并通过荧光底物分析鉴定其对组织蛋白酶 L、B 以及木瓜蛋白酶的抑制活性。通过免疫组织化学试验定位天然 HCcyst-3 蛋白。通过共孵育 rHCcyst-3 与山羊单核细胞,观察 rHCcyst-3 对细胞因子分泌、MHC 分子表达、NO 产生和吞噬作用的免疫调节作用。
我们从血矛线虫中克隆并生产了重组半胱氨酸蛋白酶抑制剂蛋白(rHCcyst-3),并研究了其对山羊单核细胞的免疫调节作用。rHCcyst-3 蛋白具有抑制组织蛋白酶 L、B 和木瓜蛋白酶活性的能力,表明其具有生物功能。免疫组织化学试验表明,天然 HCcyst-3 蛋白主要定位于线虫体表面和肠道内表面。我们证明 rHCcyst-3 可以被山羊感染血矛线虫的抗血清识别,并被山羊单核细胞摄取。结果表明,rHCcyst-3 的结合减少了 TNF-α、IL-1β 和 IL-12p40 的产生。然而,它显著增加了山羊单核细胞中 IL-10 和 TGF-β1 的分泌。rHCcyst-3 暴露后,山羊单核细胞 MHC-II 的表达受到限制。此外,rHCcyst-3 可以上调 LPS 诱导的山羊单核细胞的 NO 产生。通过 FITC-右旋糖苷内化的吞噬试验表明,rHCcyst-3 抑制了山羊单核细胞的吞噬作用。
我们的结果表明,来自血矛线虫的重组半胱氨酸蛋白酶抑制剂(rHCcyst-3)在多个方面显著调节了山羊单核细胞的功能。
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