Keyword search (4,163 papers available)

"transcriptional regulation" Keyword-tagged Publications:

Title Authors PubMed ID
1 Global survey of secondary metabolism in em Aspergillus niger /em via activation of specific transcription factors Semper C; Pham TTM; Ram S; Palys S; Evdokias G; Ouedraogo JP; Moisan MC; Geoffrion N; Reid I; Di Falco M; Bailey Z; Tsang A; Benoit-Gelber I; Savchenko A; 40852424
GENOMICS
2 Utilization of ferulic acid in Aspergillus niger requires the transcription factor FarA and a newly identified Far-like protein (FarD) that lacks the canonical Zn(II)2Cys6 domain Arentshorst M; Reijngoud J; van Tol DJC; Reid ID; Arendsen Y; Pel HJ; van Peij NNME; Visser J; Punt PJ; Tsang A; Ram AFJ; 37746181
CSFG
3 Epigenetic control of pheromone MAPK signaling determines sexual fecundity in Candida albicans. Scaduto CM, Kabrawala S, Thomson GJ, Scheving W, Ly A, Anderson MZ, Whiteway M, Bennett RJ 29255038
BIOLOGY

 

Title:Epigenetic control of pheromone MAPK signaling determines sexual fecundity in Candida albicans.
Authors:Scaduto CMKabrawala SThomson GJScheving WLy AAnderson MZWhiteway MBennett RJ
Link:https://www.ncbi.nlm.nih.gov/pubmed/29255038?dopt=Abstract
DOI:10.1073/pnas.1711141115
Publication:Proceedings of the National Academy of Sciences of the United States of America
Keywords:matingphenotypic switchingsexual reproductionsignaling bottleneckstranscriptional regulation
PMID:29255038 Category:Proc Natl Acad Sci U S A Date Added:2019-06-07
Dept Affiliation: BIOLOGY
1 Department of Molecular Microbiology and Immunology, Brown University, Providence, RI 02912.
2 Department of Biology, Concordia University, Montreal, QC, Canada H4B 1R6.
3 Department of Molecular Microbiology and Immunology, Brown University, Providence, RI 02912; Richard_Bennett@brown.edu.

Description:

Epigenetic control of pheromone MAPK signaling determines sexual fecundity in Candida albicans.

Proc Natl Acad Sci U S A. 2017 12 26;114(52):13780-13785

Authors: Scaduto CM, Kabrawala S, Thomson GJ, Scheving W, Ly A, Anderson MZ, Whiteway M, Bennett RJ

Abstract

Several pathogenic Candida species are capable of heritable and reversible switching between two epigenetic states, "white" and "opaque." In Candida albicans, white cells are essentially sterile, whereas opaque cells are mating-proficient. Here, we interrogate the mechanism by which the white-opaque switch regulates sexual fecundity and identify four genes in the pheromone MAPK pathway that are expressed at significantly higher levels in opaque cells than in white cells. These genes encode the ß subunit of the G-protein complex (STE4), the pheromone MAPK scaffold (CST5), and the two terminal MAP kinases (CEK1/CEK2). To define the contribution of each factor to mating, C. albicans white cells were reverse-engineered to express elevated, opaque-like levels of these factors, either singly or in combination. We show that white cells co-overexpressing STE4, CST5, and CEK2 undergo mating four orders of magnitude more efficiently than control white cells and at a frequency approaching that of opaque cells. Moreover, engineered white cells recapitulate the transcriptional and morphological responses of opaque cells to pheromone. These results therefore reveal multiple bottlenecks in pheromone MAPK signaling in white cells and that alleviation of these bottlenecks enables efficient mating by these "sterile" cell types. Taken together, our findings establish that differential expression of several MAPK factors underlies the epigenetic control of mating in C. albicans We also discuss how fitness advantages could have driven the evolution of a toggle switch to regulate sexual reproduction in pathogenic Candida species.

PMID: 29255038 [PubMed - indexed for MEDLINE]





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