Thind Amara C, Mota Caroline M, Gonçalves Ana Paula N, Sha Jihui, Wohlschlegel James A, Mineo Tiago W P, Bradley Peter J
bioRxiv. 2023 Jun 1:2023.05.31.543158. doi: 10.1101/2023.05.31.543158.
's propensity to infect its host and cause disease is highly dependent on its ability to modulate host cell functions. One of the strategies the parasite uses to accomplish this is via the export of effector proteins from the secretory dense granules. Dense granule (GRA) proteins are known to play roles in nutrient acquisition, host cell cycle manipulation, and immune regulation. Here, we characterize a novel dense granule protein named GRA83, which localizes to the parasitophorous vacuole in tachyzoites and bradyzoites. Disruption of results in increased virulence, weight loss, and parasitemia during the acute infection, as well as a marked increase in the cyst burden during the chronic infection. This increased parasitemia was associated with an accumulation of inflammatory infiltrates in tissues in both the acute and chronic infection. Murine macrophages infected with Δ tachyzoites produced less interleukin-12 (IL-12) , which was confirmed with reduced IL-12 and interferon gamma (IFN-γ) . This dysregulation of cytokines correlates with reduced nuclear translocation of the p65 subunit of the NF-κB complex. While GRA15 similarly regulates NF-κB, infection with Δ Δ parasites did not further reduce p65 translocation to the host cell nucleus, suggesting these GRAs function in converging pathways. We also used proximity labelling experiments to reveal candidate GRA83 interacting derived partners. Taken together, this work reveals a novel effector that stimulates the innate immune response, enabling the host to limit parasite burden.
poses a significant public health concern as it is recognized as one of the leading foodborne pathogens in the United States. Infection with the parasite can cause congenital defects in neonates, life-threatening complications in immunosuppressed patients, and ocular disease. Specialized secretory organelles, including the dense granules, play an important role in the parasite's ability to efficiently invade and regulate components of the host's infection response machinery to limit parasite clearance and establish an acute infection. s ability to avoid early clearance, while also successfully infecting the host long enough to establish a persistent chronic infection, is crucial in allowing for its transmission to a new host. While multiple GRAs directly modulate host signaling pathways, they do so in various ways highlighting the parasite's diverse arsenal of effectors that govern infection. Understanding how parasite-derived effectors harness host functions to evade defenses yet ensure a robust infection are important for understanding the complexity of the pathogen's tightly regulated infection. In this study, we characterize a novel secreted protein named GRA83 that stimulates the host cell's response to limit infection.
[寄生虫名称]感染宿主并引发疾病的倾向高度依赖于其调节宿主细胞功能的能力。寄生虫实现这一目的的策略之一是通过从分泌性致密颗粒中输出效应蛋白。已知致密颗粒(GRA)蛋白在营养获取、宿主细胞周期调控和免疫调节中发挥作用。在此,我们鉴定了一种名为GRA83的新型致密颗粒蛋白,它定位于速殖子和缓殖子的寄生泡中。[寄生虫名称]的缺失导致急性感染期间毒力增加、体重减轻和寄生虫血症,以及慢性感染期间包囊负荷显著增加。这种寄生虫血症的增加与急性和慢性感染期间组织中炎性浸润的积累有关。用缺失[寄生虫名称]的速殖子感染的小鼠巨噬细胞产生的白细胞介素-12(IL-12)减少,这在IL-12和干扰素γ(IFN-γ)减少中得到证实。细胞因子的这种失调与NF-κB复合物p65亚基的核转位减少相关。虽然GRA15同样调节NF-κB,但用缺失[寄生虫名称][寄生虫名称]的寄生虫感染并没有进一步降低p65向宿主细胞核的转位,这表明这些GRA在汇聚途径中发挥作用。我们还使用邻近标记实验来揭示候选的与GRA83相互作用的[寄生虫名称]衍生伴侣。综上所述,这项工作揭示了一种刺激先天免疫反应的新型效应蛋白,使宿主能够限制寄生虫负荷。
[寄生虫名称]是美国公认的主要食源性病原体之一,对公共卫生构成重大关注。感染该寄生虫可导致新生儿先天性缺陷、免疫抑制患者危及生命的并发症以及眼部疾病。包括致密颗粒在内的特化分泌细胞器在寄生虫有效入侵并调节宿主感染反应机制的组成部分以限制寄生虫清除并建立急性感染的能力中发挥重要作用。[寄生虫名称]避免早期清除,同时成功感染宿主足够长的时间以建立持续性慢性感染的能力,对于其传播到新宿主至关重要。虽然多种GRA直接调节宿主信号通路,但它们以各种方式进行调节,突出了寄生虫控制感染的多样效应蛋白库。了解寄生虫衍生的效应蛋白如何利用宿主功能逃避防御同时确保强大的感染,对于理解病原体严格调控的感染的复杂性很重要。在这项研究中,我们鉴定了一种名为GRA83的新型分泌蛋白,它刺激宿主细胞的反应以限制感染。
