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产毒1737的胞外蛋白质组和表面蛋白质组及其对铁限制和在人血红蛋白上生长的反应

The Exoproteome and Surfaceome of Toxigenic 1737 and Its Response to Iron Restriction and Growth on Human Hemoglobin.

作者信息

Goring Andrew K, Hale Scott, Dasika Poojita, Chen Yu, Clubb Robert T, Loo Joseph A

出版信息

J Proteome Res. 2025 Jan 3;24(1):77-93. doi: 10.1021/acs.jproteome.4c00443. Epub 2024 Dec 18.

Abstract

Toxin-producing strains are the etiological agents of the severe upper respiratory disease, diphtheria. A global phylogenetic analysis revealed that biotype gravis is particularly lethal as it produces diphtheria toxin and a range of other virulence factors, particularly when it encounters low levels of iron at sites of infection. To gain insight into how it colonizes its host, we have identified iron-dependent changes in the exoproteome and surfaceome of strain 1737 using a combination of whole-cell fractionation, intact cell surface proteolysis, and quantitative proteomics. In total, we identified 1414 of the predicted 2265 proteins (62%) encoded by its reference genome. For each protein, we quantified its degree of secretion and surface exposure, revealing that exoproteases and hydrolases predominate in the exoproteome, while the surfaceome is enriched with adhesins, particularly DIP2093. Our analysis provides insight into how components in the heme-acquisition system are positioned, showing pronounced surface exposure of the strain-specific ChtA/ChtC paralogues and high secretion of the species-conserved heme-binding HtaA protein, suggesting it functions as a hemophore. Profiling the response of the exoproteome and surfaceome after microbial exposure to human hemoglobin and iron limitation reveals potential virulence factors that may be expressed at sites of infection. Data are available via ProteomeXchange with identifier PXD051674.

摘要

产毒素菌株是严重上呼吸道疾病白喉的病原体。一项全球系统发育分析表明,重生物型特别致命,因为它会产生白喉毒素和一系列其他毒力因子,尤其是在感染部位遇到低水平铁时。为了深入了解它如何在宿主中定殖,我们使用全细胞分级分离、完整细胞表面蛋白水解和定量蛋白质组学相结合的方法,确定了1737菌株外蛋白质组和表面蛋白质组中铁依赖性的变化。我们总共鉴定出了其参考基因组预测的2265种蛋白质中的1414种(62%)。对于每种蛋白质,我们量化了其分泌程度和表面暴露程度,结果表明外蛋白酶和水解酶在外蛋白质组中占主导地位,而表面蛋白质组富含黏附素,特别是DIP2093。我们的分析揭示了血红素获取系统中的成分是如何定位的,显示出菌株特异性的ChtA/ChtC旁系同源物有明显的表面暴露,以及物种保守的血红素结合蛋白HtaA的高分泌,这表明它起到了血色素蛋白的作用。分析微生物暴露于人类血红蛋白和铁限制后外蛋白质组和表面蛋白质组的反应,揭示了可能在感染部位表达的潜在毒力因子。数据可通过ProteomeXchange获得,标识符为PXD051674。

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