Protein kinases MpkA and SepH transduce crosstalk between CWI and SIN pathways to activate protective hyphal septation under echinocandin cell wall stress.

IF 3.7 2区 生物学 Q2 MICROBIOLOGY mSphere Pub Date : 2025-01-28 Epub Date: 2024-12-13 DOI:10.1128/msphere.00641-24
Alexander G Doan, Jessica E Schafer, Casey M Douglas, Matthew S Quintanilla, Meredith E Morse, Harley Edwards, Walker D Huso, Kelsey J Gray, JungHun Lee, Joshua K Dayie, Steven D Harris, Mark R Marten
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Abstract

This study investigates a previously unreported stress signal transduced as crosstalk between the cell wall integrity (CWI) pathway and the septation initiation network (SIN). Echinocandins, which target cell wall synthesis, are widely used to treat mycoses. Their efficacy, however, is species specific. Our findings suggest that this is due largely to CWI-SIN crosstalk and the ability of filamentous species to fortify with septa in response to echinocandin stress. To better understand this crosstalk, we used a microscopy-based assay to measure septum density, aiming to understand the septation response to cell wall stress. The echinocandin micafungin, an inhibitor of β-(1,3)-glucan synthase, was employed to induce this stress. We observed a strong positive correlation between micafungin treatment and septum density in wild-type strains. This finding suggests that CWI activates SIN under cell wall stress, increasing septum density to protect against cell wall failure. More detailed investigations, with targeted knockouts of CWI and SIN signaling proteins, enabled us to identify crosstalk occurring between the CWI kinase, MpkA, and the SIN kinase, SepH. This discovery of the previously unknown crosstalk between the CWI and SIN pathways not only reshapes our understanding of fungal stress responses, but also unveils a promising new target pathway for the development of novel antifungal strategies.

Importance: Echinocandin-resistant species pose a major challenge in clinical mycology by rendering one of only four lines of treatment, notably one of the two that are well-tolerated, ineffective in treating systemic mycoses of these species. Previous studies have demonstrated that echinocandins fail against highly polarized fungi because they target only apical septal compartments. It is known that many filamentous species respond to cell wall stress with hyperseptation. In this work, we show that echinocandin resistance hinges on this dynamic response, rather than on innate septation alone. We also describe, for the first time, the signaling pathway used to deploy the hyperseptation response. By disabling this pathway, we were able to render mycelia susceptible to echinocandin stress. This work enhances our microbiological understanding of filamentous fungi and introduces a potential target to overcome echinocandin-resistant species.

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蛋白激酶MpkA和SepH介导CWI和SIN通路之间的串扰,在棘白菌素细胞壁胁迫下激活保护性菌丝分离。
本研究研究了一种以前未报道的应激信号,该信号被转导为细胞壁完整性(CWI)通路和分裂起始网络(SIN)之间的串扰。棘白菌素以细胞壁合成为靶点,被广泛用于治疗真菌病。然而,它们的功效是特定于物种的。我们的研究结果表明,这在很大程度上是由于CWI-SIN串扰和丝状物种在应对棘白菌素胁迫时加强间隔的能力。为了更好地理解这种串扰,我们使用了一种基于显微镜的方法来测量隔膜密度,旨在了解隔膜对细胞壁应力的反应。采用β-(1,3)-葡聚糖合成酶抑制剂棘白菌素micafungin诱导这种应激。我们观察到micafungin处理与野生型菌株的隔膜密度有很强的正相关。这一发现表明CWI在细胞壁应激下激活SIN,增加隔膜密度以防止细胞壁衰竭。更详细的研究,通过靶向敲除CWI和SIN信号蛋白,使我们能够确定CWI激酶MpkA和SIN激酶SepH之间发生的串扰。这一发现不仅重塑了我们对真菌胁迫反应的理解,而且为开发新的抗真菌策略揭示了一个有希望的新靶标途径。重要性:棘白菌素耐药物种对临床真菌学提出了重大挑战,因为只有四种治疗方法中的一种,特别是两种耐受性良好的治疗方法中的一种,对这些物种的系统性真菌病无效。先前的研究表明棘白菌素对高度极化的真菌不起作用,因为它们只针对根尖隔室。众所周知,许多丝状物种对细胞壁应激的反应是高渗。在这项工作中,我们表明棘白菌素耐药性取决于这种动态反应,而不仅仅是先天分离。我们还首次描述了用于部署高隔反应的信号通路。通过禁用这一途径,我们能够使菌丝体对棘白菌素的压力敏感。这项工作提高了我们对丝状真菌的微生物学认识,并引入了克服棘白菌素耐药物种的潜在靶点。
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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.
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