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BosR 和 PlzA 相互调节 RpoS 功能以维持伯氏疏螺旋体在蜱和哺乳动物中的生存。

BosR and PlzA reciprocally regulate RpoS function to sustain Borrelia burgdorferi in ticks and mammals.

机构信息

Department of Medicine, UConn Health, Farmington, Connecticut, USA.

Center for Infection and Immunity and.

出版信息

J Clin Invest. 2023 Mar 1;133(5):e166710. doi: 10.1172/JCI166710.

Abstract

The RNA polymerase alternative σ factor RpoS in Borrelia burgdorferi (Bb), the Lyme disease pathogen, is responsible for programmatic-positive and -negative gene regulation essential for the spirochete's dual-host enzootic cycle. RpoS is expressed during tick-to-mammal transmission and throughout mammalian infection. Although the mammalian-phase RpoS regulon is well described, its counterpart during the transmission blood meal is unknown. Here, we used Bb-specific transcript enrichment by tick-borne disease capture sequencing (TBDCapSeq) to compare the transcriptomes of WT and ΔrpoS Bb in engorged nymphs and following mammalian host-adaptation within dialysis membrane chambers. TBDCapSeq revealed dramatic changes in the contours of the RpoS regulon within ticks and mammals and further confirmed that RpoS-mediated repression is specific to the mammalian-phase of Bb's enzootic cycle. We also provide evidence that RpoS-dependent gene regulation, including repression of tick-phase genes, is required for persistence in mice. Comparative transcriptomics of engineered Bb strains revealed that the Borrelia oxidative stress response regulator (BosR), a noncanonical Fur family member, and the cyclic diguanosine monophosphate (c-di-GMP) effector PlzA reciprocally regulate the function of RNA polymerase complexed with RpoS. BosR is required for RpoS-mediated transcription activation and repression in addition to its well-defined role promoting transcription of rpoS by the RNA polymerase alternative σ factor RpoN. During transmission, ligand-bound PlzA antagonizes RpoS-mediated repression, presumably acting through BosR.

摘要

伯氏疏螺旋体(Bb)中的 RNA 聚合酶替代σ因子 RpoS 负责程序性的正调控和负调控,这对螺旋体的双宿主地方性循环至关重要。RpoS 在蜱向哺乳动物传播和整个哺乳动物感染过程中表达。虽然哺乳动物阶段的 RpoS 调控基因已被很好地描述,但在传播血餐期间的对应物尚不清楚。在这里,我们使用蜱传疾病捕获测序(TBDCapSeq)对 WT 和ΔrpoS Bb 在饱血的若虫和随后在透析膜室中适应哺乳动物宿主时的转录组进行了比较。TBDCapSeq 揭示了 RpoS 调控基因在蜱和哺乳动物中的轮廓发生了巨大变化,并进一步证实 RpoS 介导的抑制作用是 Bb 地方性循环的哺乳动物阶段特有的。我们还提供了证据表明,RpoS 依赖性基因调控,包括对蜱阶段基因的抑制,是在小鼠中持续存在所必需的。工程化 Bb 菌株的比较转录组学表明,伯氏螺旋体氧化应激反应调节剂(BosR),一种非典型的 Fur 家族成员,以及环状二鸟苷酸(c-di-GMP)效应物 PlzA,相互调节与 RpoS 结合的 RNA 聚合酶的功能。除了其明确的作用促进 RNA 聚合酶替代σ因子 RpoN 转录 rpoS 之外,BosR 还需要 RpoS 介导的转录激活和抑制。在传播过程中,配体结合的 PlzA 拮抗 RpoS 介导的抑制,可能通过 BosR 起作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bee6/9974103/484b982a059b/jci-133-166710-g104.jpg

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