Keyword search (4,164 papers available)

"Omran RP" Authored Publications:

Title Authors PubMed ID
1 Tri-Functional CRISPR Screen Reveals Overexpression of em QDR2 /em and em QDR3 /em Transporters Increase Fumaric Acid Production in em Kluyveromyces marxianus /em Thornbury M; Omran RP; Kumar L; Knoops A; Abushahin R; Whiteway M; Martin VJJ; 41277095
BIOLOGY
2 Candida albicans exhibits heterogeneous and adaptive cytoprotective responses to anti-fungal compounds Dumeaux V; Massahi S; Bettauer V; Mottola A; Dukovny A; Khurdia SS; Costa ACBP; Omran RP; Simpson S; Xie JL; Whiteway M; Berman J; Hallett MT; 37888959
BIOLOGY
3 A Deep Learning Approach to Capture the Essence of Candida albicans Morphologies Bettauer V; Costa ACBP; Omran RP; Massahi S; Kirbizakis E; Simpson S; Dumeaux V; Law C; Whiteway M; Hallett MT; 35972285
BIOLOGY
4 Transcriptional Profiling of the Candida albicans Response to the DNA Damage Agent Methyl Methanesulfonate Feng Y; Zhang Y; Li J; Omran RP; Whiteway M; Feng J; 35886903
BIOLOGY
5 SAGA Complex Subunits in Candida albicans Differentially Regulate Filamentation, Invasiveness, and Biofilm Formation Rashid S; Correia-Mesquita TO; Godoy P; Omran RP; Whiteway M; 35350439
BIOLOGY
6 The zinc cluster transcription factor Rha1 is a positive filamentation regulator in Candida albicans Omran RP; Ramírez-Zavala B; Aji Tebung W; Yao S; Feng J; Law C; Dumeaux V; Morschhäuser J; Whiteway M; 34849863
PERFORM
7 Signal-mediated localization of Candida albicans pheromone response pathway components Costa ACBP; Omran RP; Law C; Dumeaux V; Whiteway M; 33793759
PERFORM
8 Hof1 plays a checkpoint related role in MMS induced DNA damage response in Candida albicans. Feng J, Islam A, Bean B, Feng J, Sparapani S, Shrivastava M, Goyal A, Omran RP, Mallick J, Whiteway M 31940254
BIOLOGY
9 RNA sequencing reveals an additional Crz1-binding motif in promoters of its target genes in the human fungal pathogen Candida albicans. Xu H, Fang T, Omran RP, Whiteway M, Jiang L 31900175
BIOLOGY
10 Screening of Candida albicans GRACE library revealed a unique pattern of biofilm formation under repression of the essential gene ILS1. Costa ACBP, Omran RP, Correia-Mesquita TO, Dumeaux V, Whiteway M 31235750
PERFORM
11 MAP Kinase Regulation of the Candida albicans Pheromone Pathway. Rastghalam G, Omran RP, Alizadeh M, Fulton D, Mallick J, Whiteway M 30787119
BIOLOGY
12 Mms21: A Putative SUMO E3 Ligase in Candida albicans That Negatively Regulates Invasiveness and Filamentation, and Is Required for the Genotoxic and Cellular Stress Response. Islam A, Tebbji F, Mallick J, Regan H, Dumeaux V, Omran RP, Whiteway M 30530734
PERFORM
13 Put3 Positively Regulates Proline Utilization in Candida albicans. Tebung WA, Omran RP, Fulton DL, Morschhäuser J, Whiteway M 29242833
BIOLOGY

 

Title:SAGA Complex Subunits in Candida albicans Differentially Regulate Filamentation, Invasiveness, and Biofilm Formation
Authors:Rashid SCorreia-Mesquita TOGodoy POmran RPWhiteway M
Link:https://pubmed.ncbi.nlm.nih.gov/35350439/
DOI:10.3389/fcimb.2022.764711
Publication:Frontiers in cellular and infection microbiology
Keywords:Candida albicansSAGA acetyltransferase complexbiofilm formationfilamentationinvasivenessmacrophagesstress response
PMID:35350439 Category: Date Added:2022-03-30
Dept Affiliation: BIOLOGY
1 Department of Biology, Concordia University, Montreal, QC, Canada.

Description:

SAGA (Spt-Ada-Gcn5-acetyltransferase) is a highly conserved, multiprotein co-activator complex that consists of five distinct modules. It has two enzymatic functions, a histone acetyltransferase (HAT) and a deubiquitinase (DUB) and plays a central role in processes such as transcription initiation, elongation, protein stability, and telomere maintenance. We analyzed conditional and null mutants of the SAGA complex module components in the fungal pathogen Candida albicans; Ngg1, (the HAT module); Ubp8, (the DUB module); Tra1, (the recruitment module), Spt7, (the architecture module) and Spt8, (the TBP interaction unit), and assessed their roles in a variety of cellular processes. We observed that spt7?/? and spt8?/? strains have a filamentous phenotype, and both are highly invasive in yeast growing conditions as compared to the wild type, while ngg1?/? and ubp8?/? are in yeast-locked state and non-invasive in both YPD media and filamentous induced conditions compared to wild type. RNA-sequencing-based transcriptional profiling of SAGA mutants reveals upregulation of hyphal specific genes in spt7?/? and spt8?/? strains and downregulation of ergosterol metabolism pathway. As well, spt7?/? and spt8?/? confer susceptibility to antifungal drugs, to acidic and alkaline pH, to high temperature, and to osmotic, oxidative, cell wall, and DNA damage stresses, indicating that these proteins are important for genotoxic and cellular stress responses. Despite having similar morphological phenotypes (constitutively filamentous and invasive) spt7 and spt8 mutants displayed variation in nuclear distribution where spt7?/? cells were frequently binucleate and spt8?/? cells were consistently mononucleate. We also observed that spt7?/? and spt8?/? mutants were quickly engulfed by macrophages compared to ngg1?/? and ubp8?/? strains. All these findings suggest that the SAGA complex modules can have contrasting functions where loss of Spt7 or Spt8 enhances filamentation and invasiveness while loss of Ngg1 or Ubp8 blocks these processes.





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