A newly characterized dense granule protein (GRA76) is important for the growth and virulence of Toxoplasma gondii

IF 3.7 2区 医学 Q1 PARASITOLOGY
Xiao-Nan Zheng , Li-Xiu Sun , Hany M. Elsheikha , Ting-Ting Li , Jin Gao , Xiao-Jing Wu , Zhi-Wei Zhang , Meng Wang , Bao-Quan Fu , Xing-Quan Zhu , Jin-Lei Wang
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Abstract

Pathogenicity of the zoonotic pathogen Toxoplasma gondii largely depends on the secretion of effector proteins into the extracellular milieu and host cell cytosol, including the dense granule proteins (GRAs). The protein-encoding gene TGME49_299780 was previously identified as a contributor to parasite fitness. However, its involvement in parasite growth, virulence and infectivity in vitro and in vivo remains unknown. Here, we comprehensively examined the role of this new protein, termed GRA76, in parasite pathogenicity. Subcellular localization revealed high expression of GRA76 in tachyzoites inside the parasitophorous vacuole (PV). However, its expression was significantly decreased in bradyzoites. A CRISPR-Cas9 approach was used to knock out the gra76 gene in the T. gondii type I RH strain and type II Pru strain. The in vitro plaque assays and intracellular replication showed the involvement of GRA76 in replication of RH and Pru strains. Deletion of the gra76 gene significantly decreased parasite virulence, and reduced the brain cyst burden in mice. Using RNA sequencing, we detected a significant increase in the expression of bradyzoite-associated genes such as BAG1 and LDH2 in the PruΔgra76 strain compared with the wild-type Pru strain. Using an in vitro bradyzoite differentiation assay, we showed that loss of GRA76 significantly increased the propensity for parasites to form bradyzoites. Immunization with PruΔgra76 conferred partial protection against acute and chronic infection in mice. These findings show the important role of GRA76 in the pathogenesis of T. gondii and highlight the potential of PruΔgra76 as a candidate for a live-attenuated vaccine.

Abstract Image

Abstract Image

一种新鉴定的致密颗粒蛋白(GRA76)对弓形虫的生长和毒力具有重要意义。
人畜共患病原体弓形虫的致病性在很大程度上取决于效应蛋白分泌到细胞外环境和宿主细胞胞质溶胶中,包括致密颗粒蛋白(GRAs)。蛋白编码基因TGME49_299780先前被鉴定为寄生虫适应度的贡献者。然而,它在体外和体内对寄生虫生长、毒力和传染性的影响尚不清楚。在这里,我们全面研究了这种被称为GRA76的新蛋白质在寄生虫致病性中的作用。亚细胞定位显示GRA76在寄生液泡内的速殖子中高表达。然而,其在缓冲剂中的表达显著降低。使用CRISPR-Cas9方法敲除弓形虫I型RH菌株和II型Pru菌株中的gra76基因。体外斑块测定和细胞内复制显示GRA76参与RH和Pru菌株的复制。gra76基因的缺失显著降低了寄生虫的毒力,并降低了小鼠的脑囊肿负担。使用RNA测序,我们检测到与野生型Pru菌株相比,PruΔgra76菌株中缓激虫相关基因如BAG1和LDH2的表达显著增加。使用体外缓冲剂分化试验,我们发现GRA76的缺失显著增加了寄生虫形成缓冲剂的倾向。PruΔgra76免疫对小鼠急性和慢性感染具有部分保护作用。这些发现显示了GRA76在弓形虫发病机制中的重要作用,并突出了PruΔGRA76作为减毒活疫苗候选物的潜力。
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来源期刊
CiteScore
8.40
自引率
2.50%
发文量
76
审稿时长
23 days
期刊介绍: International Journal for Parasitology offers authors the option to sponsor nonsubscriber access to their articles on Elsevier electronic publishing platforms. For more information please view our Sponsored Articles page. The International Journal for Parasitology publishes the results of original research in all aspects of basic and applied parasitology, including all the fields covered by its Specialist Editors, and ranging from parasites and host-parasite relationships of intrinsic biological interest to those of social and economic importance in human and veterinary medicine and agriculture.
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