Identification of genome-wide binding sites of heat shock factor 1, Hsf1, under basal conditions in the human pathogenic yeast, Candida albicans

被引:0
作者
Remya Nair
Nitesh K. Khandelwal
Md. Shariq
Archana K. Redhu
Naseem A. Gaur
Shamim Shaikh
Rajendra Prasad
机构
[1] Rajiv Gandhi Institute of IT & Biotechnology,School of Life Sciences
[2] Bharati Vidyapeeth University,Department of Biosciences and Bioengineering
[3] Jawaharlal Nehru University,undefined
[4] International Centre for Genetic Engineering and Biotechnology,undefined
[5] National Institute of Pathology,undefined
[6] IIT-Bombay,undefined
[7] Amity Institute of Integrative Sciences and Health and Amity Institute of Biotechnology Amity University,undefined
来源
AMB Express | / 8卷
关键词
Hsf1 (Heat shock factor 1); Iron; Drug resistance; Heat shock; Chaperones; Motif and ;
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摘要
The master regulator of thermal stress response, Hsf1, is also an essential determinant for viability and virulence in Candida albicans. Our recent studies highlighted that apart from ubiquitous roles of Hsf1 at higher temperatures, it also has myriad non-heat shock responsive roles essential under iron deprivation and drug defense. Here, we further explored its implications in the normal cellular functioning, by profiling its genome-wide occupancy using chromatin immuno-precipitation coupled to high-density tiling arrays under basal and iron deprived conditions. Hsf1 recruitment profiles revealed that it binds to promoters of 660 genes of varied functions, under both the conditions, however, elicited variability in intensity of binding. For instance, Hsf1 binding was observed on several genes of oxidative and osmotic stress response, cell wall integrity, iron homeostasis, mitochondrial, hyphal and multidrug transporters. Additionally, the present study divulged a novel motif under basal conditions comprising, -GTGn3GTGn3GTG- where, Hsf1 displays strong occupancy at significant number of sites on several promoters distinct from the heat induced motif. Hence, by binding to and regulating major chaperones, stress responsive genes and drug resistance regulators, Hsf1 is imperative in regulating various cellular machineries. The current study provides a framework for understanding novel aspects of how Hsf1 coordinates diverse cellular functions.
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