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衣原体发育周期的计算建模揭示了不对称分裂的潜在作用。

Computational Modeling of the Chlamydial Developmental Cycle Reveals a Potential Role for Asymmetric Division.

机构信息

Department of Biological Sciences, University of Idaho, Moscow, Idaho, USA.

出版信息

mSystems. 2023 Apr 27;8(2):e0005323. doi: 10.1128/msystems.00053-23. Epub 2023 Mar 16.

Abstract

Chlamydia trachomatis is an obligate intracellular bacterium that progresses through an essential multicell form developmental cycle. Infection of the host is initiated by the elementary body (EB). Once in the host, the EB cell differentiates into the noninfectious, but replication-competent, reticulate body, or RB. After multiple rounds of replication, RBs undergo secondary differentiation, eventually producing newly infectious EBs. Here, we generated paired cell-type promoter reporter constructs and determined the kinetics of the activities of the , , and promoters. The paired constructs revealed that the developmental cycle produces at least three phenotypically distinct cell types, the RB (prom), intermediate body (IB; prom), and EB (prom). The kinetic data from the three dual-promoter constructs were used to generate two computational agent-based models to reproduce the chlamydial developmental cycle. Both models simulated EB germination, RB amplification, IB formation, and EB production but differed in the mechanism that generated the IB. The direct conversion and the asymmetric production models predicted different behaviors for the RB population, which were experimentally testable. In agreement with the asymmetric production model, RBs acted as stem cells after the initial amplification stage, producing one IB and self-renewing after every division. We also demonstrated that IBs are a transient cell population, maturing directly into EBs after formation without the need for cell division. The culmination of these results suggests that the developmental cycle can be described by a four-stage model, EB germination, RB amplification/maturation, IB production, and EB formation. Chlamydia trachomatis is an obligate intracellular bacterial pathogen responsible for both ocular and sexually transmitted infections. All are reliant on a complex developmental cycle, consisting of both infectious and noninfectious cell forms. The EB cell form initiates infection, whereas the RB cell replicates. The infectious cycle requires both cell types, as RB replication increases the cell population while EB formation disseminates the infection to new hosts. The mechanisms of RB-to-EB development are largely unknown. Here, we developed unique dual promoter reporters and used live-cell imaging and confocal microscopy to visualize the cycle at the single-cell and kinetic levels. These data were used to develop and test two agent-based models, simulating either direct conversion of RBs to EBs or production of EBs via asymmetric RB division. Our results suggest that RBs mature into a stem cell-like population producing intermediate cell forms through asymmetric division, followed by maturation of the intermediate cell type into the infectious EB. Ultimately, a more complete mechanistic understanding of the developmental cycle will lead to novel therapeutics targeting cell type development to eliminate chlamydial dissemination.

摘要

沙眼衣原体是一种必需的细胞内细菌,它经历一个基本的多细胞形式的发育周期。宿主的感染是由原体(EB)引发的。一旦进入宿主,EB 细胞分化为非感染性但具有复制能力的网状体,或 RB。经过多次复制,RBs 经历二次分化,最终产生新的感染性 EB。在这里,我们生成了配对的细胞类型启动子报告构建体,并确定了 、 和 启动子的活性动力学。配对的构建体表明,发育周期至少产生了三种表型不同的细胞类型,即 RB(prom)、中间体(IB;prom)和 EB(prom)。来自三个双启动子构建体的动力学数据用于生成两个计算代理基模型来再现衣原体的发育周期。这两个模型都模拟了 EB 的萌发、RB 的扩增、IB 的形成和 EB 的产生,但在产生 IB 的机制上有所不同。直接转化和不对称产生模型预测了 RB 群体的不同行为,这些行为可以通过实验进行测试。与不对称产生模型一致,RBs 在初始扩增阶段后充当干细胞,在每次分裂后产生一个 IB 并自我更新。我们还证明了中间体是一种短暂的细胞群体,在形成后直接成熟为 EB,而无需细胞分裂。这些结果表明,发育周期可以用一个四阶段模型来描述,即 EB 的萌发、RB 的扩增/成熟、IB 的产生和 EB 的形成。沙眼衣原体是一种必需的细胞内细菌病原体,可引起眼部和性传播感染。所有衣原体都依赖于一个复杂的发育周期,包括感染性和非感染性细胞形式。EB 细胞形式引发感染,而 RB 细胞则进行复制。感染周期需要这两种细胞类型,因为 RB 复制增加了细胞数量,而 EB 的形成则将感染传播给新的宿主。RB 到 EB 发育的机制在很大程度上尚不清楚。在这里,我们开发了独特的双启动子报告基因,并使用活细胞成像和共聚焦显微镜在单细胞和动力学水平上观察周期。这些数据被用于开发和测试两个基于代理的模型,模拟 RB 直接转化为 EB 或通过不对称 RB 分裂产生 EB。我们的结果表明,RBs 成熟为一种类似于干细胞的群体,通过不对称分裂产生中间细胞形式,然后中间细胞类型成熟为感染性 EB。最终,对发育周期的更完整的机制理解将导致针对细胞类型发育的新型治疗方法,以消除衣原体的传播。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b528/10134819/ff1dbd4d4276/msystems.00053-23-f001.jpg

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