Department of Molecular Genetics and Microbiology, School of Medicine, Duke University, Durham, North Carolina, United States of America.
University Program in Genetics and Genomics, Duke University, Durham, North Carolina, United States of America.
PLoS Pathog. 2021 Jul 9;17(7):e1009713. doi: 10.1371/journal.ppat.1009713. eCollection 2021 Jul.
Salmonella hijack host machinery in order to invade cells and establish infection. While considerable work has described the role of host proteins in invasion, much less is known regarding how natural variation in these invasion-associated host proteins affects Salmonella pathogenesis. Here we leveraged a candidate cellular GWAS screen to identify natural genetic variation in the ARHGEF26 (Rho Guanine Nucleotide Exchange Factor 26) gene that renders lymphoblastoid cells susceptible to Salmonella Typhi and Typhimurium invasion. Experimental follow-up redefined ARHGEF26's role in Salmonella epithelial cell infection. Specifically, we identified complex serovar-by-host interactions whereby ARHGEF26 stimulation of S. Typhi and S. Typhimurium invasion into host cells varied in magnitude and effector-dependence based on host cell type. While ARHGEF26 regulated SopB- and SopE-mediated S. Typhi (but not S. Typhimurium) infection of HeLa cells, the largest effect of ARHGEF26 was observed with S. Typhimurium in polarized MDCK cells through a SopB- and SopE2-independent mechanism. In both cell types, knockdown of the ARHGEF26-associated protein DLG1 resulted in a similar phenotype and serovar specificity. Importantly, we show that ARHGEF26 plays a critical role in S. Typhimurium pathogenesis by contributing to bacterial burden in the enteric fever murine model, as well as inflammation in the colitis infection model. In the enteric fever model, SopB and SopE2 are required for the effects of Arhgef26 deletion on bacterial burden, and the impact of sopB and sopE2 deletion in turn required ARHGEF26. In contrast, SopB and SopE2 were not required for the impacts of Arhgef26 deletion on colitis. A role for ARHGEF26 on inflammation was also seen in cells, as knockdown reduced IL-8 production in HeLa cells. Together, these data reveal pleiotropic roles for ARHGEF26 during infection and highlight that many of the interactions that occur during infection that are thought to be well understood likely have underappreciated complexity.
沙门氏菌劫持宿主机制以便入侵细胞并建立感染。尽管已经有大量工作描述了宿主蛋白在入侵中的作用,但对于这些与入侵相关的宿主蛋白的自然变异如何影响沙门氏菌发病机制知之甚少。在这里,我们利用候选细胞全基因组关联研究 (GWAS) 筛选来鉴定 ARHGEF26(Rho 鸟嘌呤核苷酸交换因子 26)基因中的自然遗传变异,该变异使淋巴母细胞容易感染伤寒沙门氏菌和鼠伤寒沙门氏菌。实验后续研究重新定义了 ARHGEF26 在沙门氏菌上皮细胞感染中的作用。具体来说,我们发现了复杂的血清型-宿主相互作用,即 ARHGEF26 刺激伤寒沙门氏菌和鼠伤寒沙门氏菌入侵宿主细胞的程度和效应子依赖性因宿主细胞类型而异。虽然 ARHGEF26 调节 SopB 和 SopE 介导的伤寒沙门氏菌(但不是鼠伤寒沙门氏菌)感染 HeLa 细胞,但在极化的 MDCK 细胞中,ARHGEF26 对 S. Typhimurium 的最大影响是通过 SopB 和 SopE2 独立的机制。在这两种细胞类型中,敲低 ARHGEF26 相关蛋白 DLG1 导致类似的表型和血清型特异性。重要的是,我们表明 ARHGEF26 通过在肠热病小鼠模型中有助于细菌负荷以及结肠炎感染模型中的炎症,在鼠伤寒沙门氏菌发病机制中发挥关键作用。在肠热病模型中,SopB 和 SopE2 是 Arhgef26 缺失对细菌负荷影响所必需的,而 sopB 和 sopE2 缺失的影响反过来又需要 ARHGEF26。相比之下,SopB 和 SopE2 对 Arhgef26 缺失对结肠炎的影响并不需要。ARHGEF26 在炎症中的作用也在细胞中显现出来,因为敲低导致 HeLa 细胞中 IL-8 的产生减少。总之,这些数据揭示了 ARHGEF26 在感染过程中的多效性作用,并强调了在感染过程中发生的许多被认为是众所周知的相互作用可能具有被低估的复杂性。
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