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单萜类紫苏醇通过抑制乙醛酸循环损害白色念珠菌的代谢灵活性。

Monoterpenoid perillyl alcohol impairs metabolic flexibility of Candida albicans by inhibiting glyoxylate cycle.

作者信息

Ansari Moiz A, Fatima Zeeshan, Ahmad Kamal, Hameed Saif

机构信息

Amity Institute of Biotechnology, Amity University Haryana, Gurugram (Manesar) 122413, India.

Center for Interdisciplinary Research in Basic Sciences, Jamia Millia Islamia, New Delhi 110025, India.

出版信息

Biochem Biophys Res Commun. 2018 Jan 1;495(1):560-566. doi: 10.1016/j.bbrc.2017.11.064. Epub 2017 Nov 9.

DOI:10.1016/j.bbrc.2017.11.064
PMID:29129690
Abstract

The metabolic pathway such as glyoxylate cycle (GC) enables Candida albicans, to survive under glucose deficient conditions prevalent in the hostile niche. Thus its key enzymes (Isocitrate lyase; ICL and malate synthase; MLS) represent attractive targets against C. albicans. We have previously reported the antifungal potential of a natural monoterpenoid perillyl alcohol (PA). The present study uncovers additional role of PA as a potent GC inhibitor. We explored that PA phenocopied ICL1 deletion mutant and were hypersensitive under low carbon utilizing conditions. The effect of PA on GC was substantiated by molecular docking analyses, which reveals the in-silico binding affinity of PA with ICL and MLS and explored that PA binds to the active sites of both proteins with better binding energy in comparison to their known inhibitors 3-nitropropionate and bromopyruvate respectively. Enzyme kinetics by Lineweaver-Burk plot unravels that PA inhibits ICL and MLS enzymes in competitive and non-competitive manner respectively. Moreover, semi-quantitative RT-PCR indicated that PA inhibits ICL1 and MLS1 mRNA expressions. Lastly, we demonstrated the antifungal efficacy of PA by enhanced survival of Caenorhabditis elegans model and less hemolytic activity (10.6%) on human blood cells. Further studies are warranted for PA to be considered as viable drug candidate.

摘要

乙醛酸循环(GC)等代谢途径使白色念珠菌能够在恶劣生态位中普遍存在的葡萄糖缺乏条件下存活。因此,其关键酶(异柠檬酸裂解酶;ICL和苹果酸合酶;MLS)成为抗白色念珠菌的有吸引力的靶点。我们之前报道过天然单萜紫苏醇(PA)的抗真菌潜力。本研究揭示了PA作为一种有效的GC抑制剂的额外作用。我们发现PA模拟了ICL1缺失突变体,并且在低碳利用条件下高度敏感。分子对接分析证实了PA对GC的作用,该分析揭示了PA与ICL和MLS的计算机模拟结合亲和力,并发现与已知抑制剂3-硝基丙酸和溴丙酮酸相比,PA分别以更好的结合能与这两种蛋白质的活性位点结合。通过Lineweaver-Burk图进行的酶动力学分析表明,PA分别以竞争性和非竞争性方式抑制ICL和MLS酶。此外,半定量RT-PCR表明PA抑制ICL1和MLS1 mRNA表达。最后,我们通过秀丽隐杆线虫模型的存活率提高以及对人血细胞的溶血活性较低(10.6%)证明了PA的抗真菌功效。有必要对PA进行进一步研究,以将其视为可行的药物候选物。

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