The antibacterial agent, moxifloxacin inhibits virulence factors of Candida albicans through multitargeting

被引:0
作者
Ashwini Jadhav
Bhagyashree Bansode
Datta Phule
Amruta Shelar
Rajendra Patil
Wasudev Gade
Kiran Kharat
Sankunny Mohan Karuppayil
机构
[1] School of Life Sciences (DST-FIST & UGC-SAP Sponsored),Department of Biotechnology
[2] SRTM University (NAAC Accredited with ‘A’ Grade),Department of Biotechnology
[3] Savitribai Phule Pune Univesity,undefined
[4] Deogiri College Aurangabad,undefined
来源
World Journal of Microbiology and Biotechnology | 2017年 / 33卷
关键词
Moxifloxacin; Topoisomerase; Virulence; Biofilm; Multitargeting; Yeast to hyphae transition;
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摘要
Fluoroquinolines are broad spectrum fourth generation antibiotics. Some of the Fluoroquinolines exhibit antifungal activity. We are reporting the potential mechanism of action of a fluoroquinoline antibiotic, moxifloxacin on the growth, morphogenesis and biofilm formation of the human pathogen Candida albicans. Moxifloxacin was found to be Candidacidal in nature. Moxifloxacin seems to inhibit the yeast to Hyphal morphogenesis by affecting signaling pathways. It arrested the cell cycle of C. albicans at S phase. Docking of moxifloxacin with predicted structure of C. albicans DNA Topoisomerase II suggests that moxifloxacin may bind and inhibit the activity of DNA Topoisomerase II in C. albicans. Moxifloxacin could be used as a dual purpose antibiotic for treating mixed infections caused by bacteria as well as C. albicans. In addition chances of developing moxifloxacin resistance in C. albicans are less considering the fact that moxifloxacin may target multiple steps in yeast to hyphal transition in C. albicans.
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