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硫醇过氧化物酶对于真菌病原体新型隐球菌的毒力以及对一氧化氮和过氧化物的抗性至关重要。

Thiol peroxidase is critical for virulence and resistance to nitric oxide and peroxide in the fungal pathogen, Cryptococcus neoformans.

作者信息

Missall Tricia Ann, Pusateri Mary Ellen, Lodge Jennifer K

机构信息

Edward A. Doisy Department of Biochemistry and Molecular Biology, Saint Louis University School of Medicine, 1402 S Grand Boulevard, Saint Louis, MO 63104, USA.

出版信息

Mol Microbiol. 2004 Mar;51(5):1447-58. doi: 10.1111/j.1365-2958.2004.03921.x.

Abstract

Cryptococcus neoformans is a fungal pathogen most commonly causing meningitis in immunocompromised patients. Current therapies are inadequate, and novel antifungal targets are needed. We have identified by proteomics two thiol peroxidases that are differentially expressed at 37 degrees C, the temperature of the mammalian host. Consistent with their antioxidant role, we show that the genes encoding these thiol-specific antioxidants, TSA1 and TSA3, are transcriptionally induced when C. neoformans is exposed to hydrogen peroxide. Genome sequence analysis of C. neoformans revealed a third thiol peroxidase, TSA4. We constructed single, double and triple mutants of the thiol peroxidase genes through homologous recombination and analysed their function by comparing the growth of these mutants with that of the wild-type strain. The tsa1 Delta mutant shows sensitivity to hydrogen peroxide and t-butylhydroperoxide, as well as significant growth retardation at 25 degrees C and 38.5 degrees C. The tsa1 Delta mutant is also sensitive to NO, demonstrating a link between oxidative and nitrosative stress pathways. In two mouse models of cryptococcosis, the tsa1 Delta mutant is significantly less virulent.

摘要

新型隐球菌是一种真菌病原体,最常导致免疫功能低下患者发生脑膜炎。目前的治疗方法并不充分,因此需要新的抗真菌靶点。我们通过蛋白质组学鉴定出两种硫醇过氧化物酶,它们在哺乳动物宿主的体温37摄氏度时差异表达。与它们的抗氧化作用一致,我们发现当新型隐球菌暴露于过氧化氢时,编码这些硫醇特异性抗氧化剂的基因TSA1和TSA3会被转录诱导。新型隐球菌的基因组序列分析揭示了第三种硫醇过氧化物酶TSA4。我们通过同源重组构建了硫醇过氧化物酶基因的单突变体、双突变体和三突变体,并通过比较这些突变体与野生型菌株的生长情况来分析它们的功能。tsa1Δ突变体对过氧化氢和叔丁基过氧化氢敏感,并且在25摄氏度和38.5摄氏度时生长显著迟缓。tsa1Δ突变体对一氧化氮也敏感,这表明氧化应激和亚硝化应激途径之间存在联系。在两种隐球菌病小鼠模型中,tsa1Δ突变体的毒力明显较低。

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