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新生隐球菌细胞从鼠骨髓来源的树突状细胞中的吞饮作用。

Vomocytosis of Cryptococcus neoformans cells from murine, bone marrow-derived dendritic cells.

机构信息

Department of Biomedical Engineering, University of California-Davis, Davis, CA, United States of America.

J. Crayton Pruitt Family Department of Biomedical Engineering, Gainesville, FL, United States of America.

出版信息

PLoS One. 2023 Mar 16;18(3):e0280692. doi: 10.1371/journal.pone.0280692. eCollection 2023.

Abstract

Cryptococcus neoformans (CN) cells survive within the acidic phagolysosome of macrophages (MΦ) for extended times, then escape without impacting the viability of the host cell via a phenomenon that has been coined 'vomocytosis'. Through this mechanism, CN disseminate throughout the body, sometimes resulting in a potentially fatal condition-Cryptococcal Meningitis (CM). Justifiably, vomocytosis studies have focused primarily on MΦ, as alveolar MΦ within the lung act as first responders that ultimately expel this fungal pathogen. Herein, we hypothesize that dendritic cells (DCs), an innate immune cell with attributes that include phagocytosis and antigen presentation, can also act as 'vomocytes'. Presciently, this report shows that vomocytosis of CN indeed occurs from murine, bone marrow-derived DCs. Primarily through time-lapse microscopy imaging, we show that rates of vomocytosis events from DCs are comparable to those seen from MΦ and further, are independent of the presence of the CN capsule and infection ratios. Moreover, the phagosome-altering drug bafilomycin A inhibits this phenomenon from DCs. Although DC immunophenotype does not affect the total number of vomocytic events, we observed differences in the numbers of CN per phagosome and expulsion times. Interestingly, these observations were similar in murine, bone marrow-derived MΦ. This work not only demonstrates the vomocytic ability of DCs, but also investigates the complexity of vomocytosis regulation in this cell type and MΦ under multiple modulatory conditions. Understanding the vomocytic behavior of different phagocytes and their phenotypic subtypes is needed to help elucidate the full picture of the dynamic interplay between CN and the immune system. Critically, deeper insight into vomocytosis could reveal novel approaches to treat CM, as well as other immune-related conditions.

摘要

新生隐球菌(CN)细胞在巨噬细胞(MΦ)的酸性吞噬体中存活很长时间,然后通过一种被称为“呕吐胞吐”的现象逃脱,而不会影响宿主细胞的活力。通过这种机制,CN 可以在体内传播,有时会导致潜在致命的 cryptococcal Meningitis(CM)。有理由认为,呕吐胞吐研究主要集中在 MΦ 上,因为肺部的肺泡 MΦ 是作为最终驱逐这种真菌病原体的第一道防线。在此,我们假设树突状细胞(DC)作为一种具有吞噬作用和抗原呈递作用的固有免疫细胞,也可以作为“呕吐细胞”。有先见之明的是,本报告显示 CN 的呕吐胞吐确实发生在鼠源骨髓来源的 DC 中。主要通过延时显微镜成像,我们显示 DC 的呕吐胞吐事件率与 MΦ 中观察到的相似,并且与 CN 荚膜的存在和感染比例无关。此外,吞噬体改变药物巴佛洛霉素 A 抑制了这种现象在 DC 中的发生。尽管 DC 免疫表型不影响总呕吐胞吐事件数,但我们观察到每个吞噬体中的 CN 数量和排出时间的差异。有趣的是,在鼠源骨髓来源的 MΦ 中观察到了类似的现象。这项工作不仅证明了 DC 的呕吐胞吐能力,还研究了在多种调节条件下该细胞类型和 MΦ 中呕吐胞吐调节的复杂性。了解不同吞噬细胞及其表型亚型的呕吐胞吐行为对于阐明 CN 与免疫系统之间动态相互作用的全貌是必要的。深入了解呕吐胞吐作用可以揭示治疗 CM 以及其他免疫相关疾病的新方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4242/10019626/773d5e514042/pone.0280692.g001.jpg

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