Shwab E Keats, Juvvadi Praveen R, Waitt Greg, Soderblom Erik J, Moseley M Arthur, Nicely Nathan I, Asfaw Yohannes G, Steinbach William J
Division of Pediatric Infectious Diseases, Department of Pediatrics, Duke University Medical Center, Durham, North Carolina, USA.
Duke Proteomics and Metabolomics Core Facility, Center for Genomic and Computational Biology, Duke University, Durham, North Carolina, USA.
mBio. 2017 Feb 7;8(1):e02319-16. doi: 10.1128/mBio.02319-16.
Invasive aspergillosis (IA), caused by the filamentous fungal pathogen Aspergillus fumigatus, is a major cause of death among immunocompromised patients. The cyclic AMP/protein kinase A (PKA) signaling pathway is essential for hyphal growth and virulence of A. fumigatus, but the mechanism of regulation of PKA remains largely unknown. Here, we discovered a novel mechanism for the regulation of PKA activity in A. fumigatus via phosphorylation of key residues within the major catalytic subunit, PkaC1. Phosphopeptide enrichment and tandem mass spectrometry revealed the phosphorylation of PkaC1 at four sites (S175, T331, T333, and T337) with implications for important and diverse roles in the regulation of A. fumigatus PKA. While the phosphorylation at one of the residues (T333) is conserved in other species, the identification of three other residues represents previously unknown PKA phosphoregulation in A. fumigatus Site-directed mutagenesis of the phosphorylated residues to mimic or prevent phosphorylation revealed dramatic effects on kinase activity, growth, conidiation, cell wall stress response, and virulence in both invertebrate and murine infection models. Three-dimensional structural modeling of A. fumigatus PkaC1 substantiated the positive or negative regulatory roles for specific residues. Suppression of PKA activity also led to downregulation of PkaC1 protein levels in an apparent novel negative-feedback mechanism. Taken together, we propose a model in which PkaC1 phosphorylation both positively and negatively modulates its activity. These findings pave the way for future discovery of fungus-specific aspects of this key signaling network.
Our understanding of signal transduction networks in pathogenic fungi is limited, despite the increase in invasive fungal infections and rising mortality rates in the immunosuppressed patient population. Because PKA is known to be essential for hyphal growth and virulence of A. fumigatus, we sought to identify fungus-specific regulatory mechanisms governing PKA activity. In this study, we identify, for the first time, a novel mechanism for the regulation of PKA signaling in which differential phosphorylation of the PkaC1 catalytic subunit can lead to either positive or negative regulation of activity. Furthermore, we show that inactivation of PKA signaling leads to downregulation of catalytic subunit protein levels in a negative-feedback mechanism distinct from expression patterns previously reported in the yeasts. Our findings represent a divergence in the regulation of PKA signaling in A. fumigatus, which could potentially be exploited as a target and also open the avenue for discovery of fungus-specific downstream effectors of PKA.
侵袭性曲霉病(IA)由丝状真菌病原体烟曲霉引起,是免疫功能低下患者死亡的主要原因。环磷酸腺苷/蛋白激酶A(PKA)信号通路对烟曲霉的菌丝生长和毒力至关重要,但PKA的调节机制在很大程度上仍不清楚。在这里,我们发现了一种通过主要催化亚基PkaC1内关键残基的磷酸化来调节烟曲霉中PKA活性的新机制。磷酸肽富集和串联质谱分析揭示了PkaC1在四个位点(S175、T331、T333和T337)的磷酸化,这对烟曲霉PKA调节中的重要和多样作用具有影响。虽然其中一个残基(T333)的磷酸化在其他物种中是保守的,但另外三个残基的鉴定代表了烟曲霉中以前未知的PKA磷酸调节。将磷酸化残基定点突变为模拟或阻止磷酸化,在无脊椎动物和小鼠感染模型中均对激酶活性、生长、分生孢子形成、细胞壁应激反应及毒力产生显著影响。烟曲霉PkaC1的三维结构建模证实了特定残基的正向或负向调节作用。PKA活性的抑制还导致PkaC1蛋白水平在一种明显的新型负反馈机制中下调。综上所述,我们提出了一个模型,其中PkaC1磷酸化对其活性具有正向和负向调节作用。这些发现为未来发现这个关键信号网络中真菌特异性方面铺平了道路。
尽管侵袭性真菌感染增加且免疫抑制患者群体死亡率上升,但我们对致病真菌信号转导网络的了解仍然有限。由于已知PKA对烟曲霉的菌丝生长和毒力至关重要,我们试图确定控制PKA活性的真菌特异性调节机制。在本研究中,我们首次确定了一种调节PKA信号的新机制,其中PkaC1催化亚基的差异磷酸化可导致活性的正向或负向调节。此外,我们表明PKA信号失活会导致催化亚基蛋白水平在一种不同于先前在酵母中报道的表达模式的负反馈机制中下调。我们的发现代表了烟曲霉中PKA信号调节的差异,这可能被用作一个靶点,也为发现PKA的真菌特异性下游效应物开辟了道路。
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