An unusual Toll/MyD88-mediated Drosophila host defence against Talaromyces marneffei.

IF 2.4 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Fly Pub Date : 2024-12-01 Epub Date: 2024-09-06 DOI:10.1080/19336934.2024.2398300
Xiaoyue Wang, Qinglin Qu, Zi Li, Sha Lu, Dominique Ferrandon, Liyan Xi
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引用次数: 0

Abstract

Talaromycosis, caused by Talaromyces marneffei (T. marneffei, formerly known as Penicillium marneffei), is an opportunistic invasive mycosis endemic in tropical and subtropical areas of Asia with high mortality rate. Despite various infection models established to study the immunological interaction between T. marneffei and the host, the pathogenicity of this fungus is not yet fully understood. So far, Drosophila melanogaster, a well-established genetic model organism to study innate immunity, has not been used in related research on T. marneffei. In this study, we provide the initial characterization of a systemic infection model of T. marneffei in the D. melanogaster host. Survival curves and fungal loads were tested as well as Toll pathway activation was quantified by RT-qPCR of several antimicrobial peptide (AMP) genes including Drosomycin, Metchnikowin, and Bomanin Short 1. We discovered that whereas most wild-type flies were able to overcome the infection, MyD88 or Toll mutant flies failed to prevent fungal dissemination and proliferation and ultimately succumbed to this challenge. Unexpectedly, the induction of classical Toll pathway activation readouts, Drosomycin and Bomanin Short 1, by live or killed T. marneffei was quite limited in wild-type flies, suggesting that the fungus largely escapes detection by the systemic immune system. This unusual situation of a poor systemic activation of the Toll pathway and a strong susceptibility phenotype of MyD88/Toll might be accounted for by a requirement for this host defence in only specific tissues, a hypothesis that remains to be rigorously tested.

一种不寻常的 Toll/MyD88 介导的果蝇宿主防御马拉尼菲氏菌(Talaromyces marneffei)的方法。
由马内菲塔拉霉菌(T. marneffei,原名马内菲青霉)引起的塔拉菌病是亚洲热带和亚热带地区流行的一种机会性侵袭真菌病,死亡率很高。尽管已经建立了多种感染模型来研究马内菲青霉与宿主之间的免疫相互作用,但人们对这种真菌的致病性还不完全了解。黑腹果蝇是研究先天性免疫的一种成熟的遗传模式生物,但迄今为止还没有被用于马内菲氏菌的相关研究。在本研究中,我们初步确定了黑腹果蝇宿主中 T. marneffei 系统感染模型的特征。我们测试了存活曲线和真菌负荷,并通过 RT-qPCR 对包括 Drosomycin、Metchnikowin 和 Bomanin Short 1 在内的多个抗菌肽(AMP)基因进行了定量分析。我们发现,虽然大多数野生型苍蝇都能克服感染,但 MyD88 或 Toll 突变体苍蝇却无法阻止真菌的传播和增殖,并最终屈服于这一挑战。意想不到的是,野生型苍蝇在活体或杀死的 T. marneffei 真菌诱导经典 Toll 通路活化读数(Drosomycin 和 Bomanin Short 1)时受到很大限制,这表明该真菌在很大程度上逃避了系统免疫系统的检测。这种 Toll 通路系统激活能力差而 MyD88/Toll 易感表型强的不寻常情况可能是由于只有特定组织需要这种宿主防御系统,这一假设还有待严格检验。
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来源期刊
Fly
Fly 生物-生化与分子生物学
CiteScore
2.90
自引率
0.00%
发文量
17
审稿时长
>12 weeks
期刊介绍: Fly is the first international peer-reviewed journal to focus on Drosophila research. Fly covers a broad range of biological sub-disciplines, ranging from developmental biology and organogenesis to sensory neurobiology, circadian rhythm and learning and memory, to sex determination, evolutionary biology and speciation. We strive to become the “to go” resource for every researcher working with Drosophila by providing a forum where the specific interests of the Drosophila community can be discussed. With the advance of molecular technologies that enable researchers to manipulate genes and their functions in many other organisms, Fly is now also publishing papers that use other insect model systems used to investigate important biological questions. Fly offers a variety of papers, including Original Research Articles, Methods and Technical Advances, Brief Communications, Reviews and Meeting Reports. In addition, Fly also features two unconventional types of contributions, Counterpoints and Extra View articles. Counterpoints are opinion pieces that critically discuss controversial papers questioning current paradigms, whether justified or not. Extra View articles, which generally are solicited by Fly editors, provide authors of important forthcoming papers published elsewhere an opportunity to expand on their original findings and discuss the broader impact of their discovery. Extra View authors are strongly encouraged to complement their published observations with additional data not included in the original paper or acquired subsequently.
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