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在关键乙醛酸循环酶中存在烟曲霉缺失突变体的中性粒细胞减少小鼠中,在脂质上生长的能力决定了其完全致病表型。

Ability to grow on lipids accounts for the fully virulent phenotype in neutropenic mice of Aspergillus fumigatus null mutants in the key glyoxylate cycle enzymes.

作者信息

Olivas Israel, Royuela Mar, Romero Beatriz, Monteiro M Cândida, Mínguez José M, Laborda Fernando, De Lucas J Ramón

机构信息

Departamento de Microbiología y Parasitología, Universidad de Alcalá, Carretera Madrid-Barcelona Km 33, Alcalá de Henares, ES-28871 Madrid, Spain.

出版信息

Fungal Genet Biol. 2008 Jan;45(1):45-60. doi: 10.1016/j.fgb.2007.05.002. Epub 2007 Jun 2.

Abstract

Incidence and mortality rates of invasive aspergillosis clearly indicate the need of novel antifungals to treat patients suffering from this disease. Fungal proteins playing a crucial role in pathogenesis and with no orthologue in human cells are considered as primary therapeutic targets for the development of new antifungals with a high therapeutic index, one of the major drawbacks of the standard antifungal therapy, so far. In this work, we have analyzed the role in pathogenesis of the key enzymes of the Aspergillus fumigatus glyxoxylate cycle, isocitrate lyase and malate synthase, two possible candidates to primary therapeutic targets in this fungus. Deletion strains lacking isocitrate lyase (DeltaacuD strains) or malate synthase (DeltaacuE mutants) were constructed in this work. The Neurospora crassa pyr-4 gene was used as the replacing marker in gene deletion experiments. The pathogenicities of DeltaacuD and DeltaacuE mutants were tested in neutropenic mice and compared with those of two reference wild-type isolates A. fumigatus 237 and A. fumigatus 293. Interestingly, virulence and cytological studies clearly indicated the dispensability of the A. fumigatus glyoxylate cycle for pathogenicity. In addition, these results suggested the suitability of the pyr-4 gene as a valuable replacing marker for virulence studies in this fungus, a fact that was further confirmed by gene expression analyses. Finally, growth tests were performed to investigate the germination and growth of the DeltaacuD and DeltaacuE strains in nutrient deprivation environments, resembling the conditions that A. fumigatus conidia face after phagocytosis. Results obtained in this work strongly suggest that the ability to grow on lipids (triglycerides) of A. fumigatus isocitrate lyase and malate synthase deletion strains accounts for their fully virulent phenotype.

摘要

侵袭性曲霉病的发病率和死亡率清楚地表明,需要新型抗真菌药物来治疗患有这种疾病的患者。在发病机制中起关键作用且在人类细胞中无直系同源物的真菌蛋白被视为开发具有高治疗指数的新型抗真菌药物的主要治疗靶点,而高治疗指数是迄今为止标准抗真菌治疗的主要缺点之一。在这项工作中,我们分析了烟曲霉乙醛酸循环的关键酶异柠檬酸裂解酶和苹果酸合酶在发病机制中的作用,这两种酶是该真菌主要治疗靶点的两个可能候选者。在这项工作中构建了缺乏异柠檬酸裂解酶的缺失菌株(ΔacuD菌株)或缺乏苹果酸合酶的突变体(ΔacuE突变体)。在基因缺失实验中,使用粗糙脉孢菌pyr-4基因作为替代标记。在中性粒细胞减少的小鼠中测试了ΔacuD和ΔacuE突变体的致病性,并与两种参考野生型分离株烟曲霉237和烟曲霉293的致病性进行了比较。有趣的是,毒力和细胞学研究清楚地表明烟曲霉乙醛酸循环对于致病性是可有可无的。此外,这些结果表明pyr-4基因适合作为该真菌毒力研究的有价值的替代标记,基因表达分析进一步证实了这一事实。最后,进行了生长试验,以研究ΔacuD和ΔacuE菌株在营养剥夺环境中的萌发和生长情况,这种环境类似于烟曲霉分生孢子在吞噬作用后面临的条件。这项工作中获得的结果强烈表明,烟曲霉异柠檬酸裂解酶和苹果酸合酶缺失菌株在脂质(甘油三酯)上生长的能力是其完全毒力表型的原因。

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