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Genome‐wide analysis of the regulation of Cu metabolism in Cryptococcus neoformans Cryptococcus neoformans

机译:Cutpoccus Neoformans Cryptococccus Neoformans中Cu代谢调控的基因组分析

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Summary The ability of the human fungal pathogen Cryptococcus neoformans to adapt to variable copper (Cu) environments within the host is key for successful dissemination and colonization. During pulmonary infection, host alveolar macrophages compartmentalize Cu into the phagosome and C. neoformans Cu‐detoxifying metallothioneins, MT1 and MT2, are required for survival of the pathogen. In contrast, during brain colonization the C. neoformans Cu + importers Ctr1 and Ctr4 are required for virulence. Central for the regulation and expression of both the Cu detoxifying MT1/2 and the Cu acquisition Ctr1/4 proteins is the Cu‐metalloregulatory transcription factor Cuf1, an established C. neoformans virulence factor. Due to the importance of the distinct C. neoformans Cu homeostasis mechanisms during host colonization and virulence, and to the central role of Cuf1 in regulating Cu homeostasis, we performed a combination of RNA‐Seq and ChIP‐Seq experiments to identify differentially transcribed genes between conditions of high and low Cu. We demonstrate that the transcriptional regulation exerted by Cuf1 is intrinsically complex and that Cuf1 also functions as a transcriptional repressor. The Cu‐ and Cuf1‐dependent regulon in C. neoformans reveals new adaptive mechanisms for Cu homeostasis in this pathogenic fungus and identifies potential new pathogen‐specific targets for therapeutic intervention in fungal infections.
机译:发明内容人类真菌病原体碱基加入能量的能力适应宿主内的可变铜(CU)环境是成功传播和定植的关键。在肺部感染期间,宿主肺泡巨噬细胞将Cu分离成吞噬物体和C. Neoformans Cu-解毒金属噻吩,MT1和MT2是病原体的存活所必需的。相反,在脑结肠期间,毒力需要C. Neoformans Cu +进口商Ctr1和Ctr4。 Cu解毒MT1 / 2的调节和表达的中心是Cu-Metalloreculatory转录因子Cuf1,其已建立的C.Neoformans毒力因子。由于在宿主定植和毒力期间不同的C.Neoformans Cu稳态机制的重要性,以及CUF1在调节Cu稳态中的核心作用,我们进行了RNA-SEQ和芯片-SEQ实验的组合,以鉴定差异转录的基因高低铜的条件。我们证明CUF1施加的转录调节本质上是复杂的,并且CUF1也用作转录压缩机。 C.Neoformans中的Cu-和Cuf1依赖性调节件揭示了这种致病真菌中Cu稳态的新自适应机制,并鉴定了用于真菌感染的治疗干预的潜在新的病原体特异性靶标。

著录项

  • 来源
    《Molecular Microbiology》 |2018年第5期|共22页
  • 作者单位

    Department of Pharmacology and Cancer BiologyDuke University School of MedicineDurham NC USA;

    Department of Pharmacology and Cancer BiologyDuke University School of MedicineDurham NC USA;

    Department of Pharmacology and Cancer BiologyDuke University School of MedicineDurham NC USA;

    Division of Infectious Diseases Department of MedicineDuke University School of MedicineDurham NC;

    Department of Pharmacology and Cancer BiologyDuke University School of MedicineDurham NC USA;

    Department of Pharmacology and Cancer BiologyDuke University School of MedicineDurham NC USA;

    Department of Biochemistry and BiophysicsUCSFSan Francisco CA USA;

    Department of GeneticsYale University School of MedicineNew Haven CT USA;

    Department of GeneticsYale University School of MedicineNew Haven CT USA;

    Department of Biochemistry and BiophysicsUCSFSan Francisco CA USA;

    Division of Infectious Diseases Department of MedicineDuke University School of MedicineDurham NC;

    Department of Pharmacology and Cancer BiologyDuke University School of MedicineDurham NC USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
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