Burkholderia pseudomallei BopE suppresses the Rab32-dependent defense pathway to promote its intracellular replication and virulence.

IF 3.7 2区 生物学 Q2 MICROBIOLOGY mSphere Pub Date : 2024-11-21 Epub Date: 2024-10-21 DOI:10.1128/msphere.00453-24
Chenglong Rao, Ziyuan Zhang, Jianpeng Qiao, Dongqi Nan, Pan Wu, Liting Wang, Changhao Yao, Senquan Zheng, Jinzhu Huang, Yaling Liao, Wenzheng Liu, Zhiqiang Hu, Shiwei Wang, Yuan Wen, Jingmin Yan, Xuhu Mao, Qian Li
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Abstract

Melioidosis is a serious infectious disease caused by the Gram-negative bacterium Burkholderia pseudomallei. Recently, Rab32-dependent immune vesicles emerge as a critical defense pathway to restrict the intracellular B. pseudomallei. However, B. pseudomallei can evade host immune vesicles and survive in the cytoplasm, although this mechanism is not well understood. In this study, we found Rab32-dependent vesicles could effectively combat B. pseudomallei infection, but not all intracellular B. pseudomallei were encapsulated in Rab32-positive vesicles. To explore how B. pseudomallei counteracted the Rab32-dependent defense pathway, transcriptomic profiling of B. pseudomallei was performed to characterize the response dynamics during infection. We found that the type III secretion system of B. pseudomallei was activated, and a variety of effector proteins were highly upregulated. Among them, BopE, BprD, and BipC were shown to interact with Rab32. Interestingly, BopE directly interacts with host Rab32, potentially suppressing Rab32 function by interfering with nucleotide exchange, which in turn restricts the recruitment of Rab32 to bacterial-containing vesicles. Knocking out of BopE can increase the proportion of Rab32-positive vesicles, suppressing the intracellular replication and virulence of B. pseudomallei. Collectively, our findings have demonstrated that BopE may be an important effector for B. pseudomallei to evade from the Rab32-dependent killing vesicles into the cytosol for survival and replication. Therefore, a deeper understanding of the interaction between BopE and the host Rab32-dependent restriction pathway may provide an effective therapeutic strategy for the elimination of intracellular B. pseudomallei.IMPORTANCEB. pseudomallei is facultative intracellular bacterium that has evolved numerous strategies to evade host immune vesicles and survive in the cytoplasm. Rab32-dependent vesicles are one of these immune vesicles, but the mechanism by which B. pseudomallei escape Rab32-dependent vesicles remains elusive. Here, we find B. pseudomallei infection leading the activation of the type III secretion system (T3SS-3) and increasing the expression of various effectors. Specifically, we identify that BopE, an effector secreted by T3SS-3, triggers vesicle escape to promote B. pseudomallei pathogenicity and survival. Mechanistically, BopE suppresses the activation of Rab32 by interfering with nucleotide exchange, ultimately triggering vesicle escape and intracellular survival. We also find knocking out the bopE gene can increase the proportion of Rab32-positive vesicles that trap B. pseudomallei, dampening the survival of B. pseudomallei both in vitro and in vivo. Taken together, our findings provide insights into the molecular mechanisms of pathogen effector-induced vesicle escape, indicating a potential melioidosis treatment via blocking B. pseudomallei BopE-host Rab32 interaction.

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假丝酵母伯克霍尔德菌 BopE 可抑制 Rab32 依赖性防御途径,从而促进其胞内复制和毒力。
美拉德氏病是由革兰氏阴性伯克霍尔德氏假丝酵母菌(Burkholderia pseudomallei)引起的一种严重传染病。最近,Rab32 依赖性免疫囊泡成为限制假丝酵母菌进入细胞内的关键防御途径。然而,假丝酵母菌可以躲避宿主的免疫囊泡,并在细胞质中存活,但这一机制尚不十分清楚。在这项研究中,我们发现依赖于Rab32的囊泡能有效对抗假丝酵母菌感染,但并非所有细胞内的假丝酵母菌都被包裹在Rab32阳性囊泡中。为了探索假丝酵母如何对抗依赖于Rab32的防御途径,我们对假丝酵母进行了转录组分析,以描述感染期间的反应动态。我们发现,假丝酵母菌的Ⅲ型分泌系统被激活,多种效应蛋白高度上调。其中,BopE、BprD 和 BipC 与 Rab32 相互作用。有趣的是,BopE直接与宿主Rab32相互作用,可能通过干扰核苷酸交换来抑制Rab32的功能,进而限制Rab32被招募到含细菌的囊泡中。敲除 BopE 可增加 Rab32 阳性囊泡的比例,从而抑制假丝酵母菌的胞内复制和毒力。总之,我们的研究结果表明,BopE可能是假丝酵母菌从依赖Rab32的杀伤囊泡中逃逸到细胞质中生存和复制的重要效应物。因此,深入了解 BopE 与宿主 Rab32 依赖性限制通路之间的相互作用,可能会为消除细胞内假丝状酵母菌提供有效的治疗策略。Rab32依赖性囊泡是这些免疫囊泡之一,但假丝酵母菌逃避Rab32依赖性囊泡的机制仍然难以捉摸。在这里,我们发现假丝酵母菌感染会导致 III 型分泌系统(T3SS-3)的激活,并增加各种效应物的表达。具体来说,我们发现由 T3SS-3 分泌的效应物 BopE 会触发囊泡逃逸,从而促进假丝酵母菌的致病性和存活。从机理上讲,BopE 通过干扰核苷酸交换抑制 Rab32 的活化,最终引发囊泡逃逸和细胞内存活。我们还发现,敲除 bopE 基因可增加捕获假丝酵母的 Rab32 阳性囊泡的比例,从而抑制假丝酵母在体外和体内的存活。总之,我们的研究结果为病原体效应物诱导囊泡逃逸的分子机制提供了见解,表明通过阻断B. pseudomallei BopE与宿主Rab32的相互作用有可能治疗类鼻疽。
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来源期刊
mSphere
mSphere Immunology and Microbiology-Microbiology
CiteScore
8.50
自引率
2.10%
发文量
192
审稿时长
11 weeks
期刊介绍: mSphere™ is a multi-disciplinary open-access journal that will focus on rapid publication of fundamental contributions to our understanding of microbiology. Its scope will reflect the immense range of fields within the microbial sciences, creating new opportunities for researchers to share findings that are transforming our understanding of human health and disease, ecosystems, neuroscience, agriculture, energy production, climate change, evolution, biogeochemical cycling, and food and drug production. Submissions will be encouraged of all high-quality work that makes fundamental contributions to our understanding of microbiology. mSphere™ will provide streamlined decisions, while carrying on ASM''s tradition for rigorous peer review.
期刊最新文献
Shining a light on Candida-induced epithelial damage with a luciferase reporter. Strain variation in Candida albicans glycolytic gene regulation. The putative type 4 secretion system effector BspD is involved in maintaining envelope integrity of the pathogen Brucella. Burkholderia pseudomallei BopE suppresses the Rab32-dependent defense pathway to promote its intracellular replication and virulence. Chlamydia trachomatis Inc Ct226 is vital for FLI1 and LRRF1 recruitment to the chlamydial inclusion.
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