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金黄色葡萄球菌 fadXDEBA 基因座是代谢外源性棕榈酸和体内生长所必需的。

The fadXDEBA locus of Staphylococcus aureus is required for metabolism of exogenous palmitic acid and in vivo growth.

机构信息

Department of Microbiology and Immunology, University of Western Ontario, London, Ontario, Canada.

Chemical Engineering and Applied Chemistry, University of Toronto, Toronto, Ontario, Canada.

出版信息

Mol Microbiol. 2023 Sep;120(3):425-438. doi: 10.1111/mmi.15131. Epub 2023 Jul 27.

Abstract

In Staphylococcus aureus, genes that should confer the capacity to metabolize fatty acids by β-oxidation occur in the fadXDEBA locus, but their function has not been elucidated. Previously, incorporation into phospholipid through the fatty acid kinase FakA pathway was thought to be the only option available for S. aureus to metabolize exogenous saturated fatty acids. We now find that in S. aureus USA300, a fadX::lux reporter was repressed by glucose and induced by palmitic acid but not stearic acid, while in USA300ΔfakA basal expression was significantly elevated, and enhanced in response to both fatty acids. When cultures were supplemented with palmitic acid, palmitoyl-CoA representing the first metabolite in the β-oxidation pathway was detected in USA300, but not in a fadXDEBA deletion mutant USA300Δfad, which relative to USA300 exhibited increased incorporation of palmitic acid into phospholipid accompanied by a rapid loss of viability. USA300Δfad also exhibited significantly reduced viability in a murine tissue abscess infection model. Our data are consistent with FakA-mediated incorporation of fatty acids into phospholipid as a preferred pathway for metabolism of exogenous fatty acids, while the fad locus is critical for metabolism of palmitic acid, which is the most abundant free fatty acid in human plasma.

摘要

在金黄色葡萄球菌中,通过β-氧化代谢脂肪酸的基因存在于 fadXDEBA 基因座中,但它们的功能尚未阐明。此前,通过脂肪酸激酶 FakA 途径掺入磷脂被认为是金黄色葡萄球菌代谢外源性饱和脂肪酸的唯一选择。我们现在发现,在金黄色葡萄球菌 USA300 中, fadX::lux 报告基因被葡萄糖抑制,被棕榈酸诱导,但不受硬脂酸诱导,而在 USA300ΔfakA 中,基础表达显著升高,并对两种脂肪酸都有增强的反应。当培养物中添加棕榈酸时,在 USA300 中检测到了β-氧化途径的第一个代谢产物棕榈酰-CoA,但在 fadXDEBA 缺失突变体 USA300Δfad 中没有检测到,与 USA300 相比,USA300Δfad 将更多的棕榈酸掺入磷脂,同时迅速丧失活力。USA300Δfad 在小鼠组织脓肿感染模型中的活力也显著降低。我们的数据与 FakA 介导的将脂肪酸掺入磷脂作为代谢外源性脂肪酸的首选途径一致,而 fad 基因座对于棕榈酸的代谢至关重要,棕榈酸是人体血浆中最丰富的游离脂肪酸。

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