Jiangsu Key Laboratory of Marine Biotechnology, College of Marine Life and Fisheries, Jiangsu Ocean University, Lianyungang, China.
Co-Innovation Center of Jiangsu Marine Bio-industry Technology, Lianyungang, China.
Front Cell Infect Microbiol. 2020 Feb 14;10:53. doi: 10.3389/fcimb.2020.00053. eCollection 2020.
is found to be an important facultative intracellular pathogen with a broad host range. These organisms can replicate and survive within host macrophages to escape from the subversion of the immune defense. -macrophage interaction is very important in determining the outcome of edwardsiellasis. As an effector protein of T6SS, EvpP has been determined to be a very important virulence factor for , although its precise role in -macrophage interactions is not yet clear. In this study, the roles of EvpP in -macrophage interactions were characterized. Here, we constructed the deletion mutants of P (ΔP) and complementation (ΔP-C) by the allelic exchange method. Compared to wild type strain (WT), ΔP was found to be attenuated for growth within macrophages. In line with this observation, we found its survival capacity was lower than WT under oxidative and acid stress , which simulate conditions encountered in host macrophages. Attenuation of ΔP also correlated with enhanced activation of macrophages, as reflected by augmented NO production in ΔP-treated macrophages. Moreover, compared to WT, ΔP induced markedly increased apoptosis of macrophages, characterized by increased Annexin V binding and the activation of cleaved caspase-3. These findings provided strong evidence that EvpP is involved in the process of macrophage interactions and is required for its survival and replication in macrophages. Thus, we propose that EvpP might be an important factor that controlling the fate of inside macrophages. To further exploring the underlying mechanism of EvpP action, the cDNA library was constructed from -infected macrophages and a yeast two-hybrid screen was performed to search for cellular proteins interacting with EvpP. Ribosomal protein S5 (RPS5) was identified as a target of EvpP. Furthermore, the interaction was validated with co-immunoprecipitation assay. This result implies that the observed effect of EvpP on macrophages might be related to RPS5-mediated regulation, contributing to a better understanding of the mechanisms of EvpP involved in -macrophage interactions.
被发现是一种重要的兼性细胞内病原体,具有广泛的宿主范围。这些生物体可以在宿主巨噬细胞内复制和存活,从而逃避免疫防御的破坏。-巨噬细胞相互作用在确定爱德华氏菌病的结果方面非常重要。作为 T6SS 的效应蛋白,EvpP 已被确定为爱德华氏菌的一个非常重要的毒力因子,尽管其在-巨噬细胞相互作用中的精确作用尚不清楚。在这项研究中,我们对 EvpP 在-巨噬细胞相互作用中的作用进行了表征。在这里,我们通过等位基因交换方法构建了 P 的缺失突变体(ΔP)和互补(ΔP-C)。与野生型菌株(WT)相比,ΔP 在巨噬细胞内的生长能力减弱。与这一观察结果一致,我们发现它在氧化和酸性应激下的存活能力低于 WT,这模拟了宿主巨噬细胞中遇到的条件。ΔP 的衰减也与巨噬细胞的激活增强有关,这反映在ΔP 处理的巨噬细胞中 NO 产生增加。此外,与 WT 相比,ΔP 诱导的巨噬细胞凋亡明显增加,特征为 Annexin V 结合增加和 cleaved caspase-3 的激活。这些发现提供了强有力的证据表明 EvpP 参与了巨噬细胞相互作用的过程,并且是其在巨噬细胞中存活和复制所必需的。因此,我们提出 EvpP 可能是控制细菌在巨噬细胞内命运的重要因素。为了进一步探索 EvpP 作用的潜在机制,从感染的巨噬细胞中构建了 cDNA 文库,并进行了酵母双杂交筛选,以寻找与 EvpP 相互作用的细胞蛋白。核糖体蛋白 S5(RPS5)被鉴定为 EvpP 的靶标。此外,通过共免疫沉淀实验验证了相互作用。这一结果表明,EvpP 对巨噬细胞的影响可能与 RPS5 介导的调节有关,有助于更好地理解 EvpP 参与-巨噬细胞相互作用的机制。
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