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HOME > J. Microbiol > Volume 56(10); 2018 > Article
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Roles of eIF4E-binding protein Caf20 in Ste12 translation and P-body formation in yeast
Kiyoung Park , Yu-Seon Lee , Daehee Jung , Jinmi Kim
Journal of Microbiology 2018;56(10):744-747.
DOI: https://doi.org/10.1007/s12275-018-8230-0
Published online: August 22, 2018
Department of Microbiology and Molecular Biology, College of Bioscience and Biotechnology, Chungnam National University, Daejeon 34134, Republic of Korea
Corresponding author:  Jinmi Kim , Tel: +82-42-821-6416;, 
Received: 30 April 2018   • Revised: 9 July 2018   • Accepted: 10 July 2018
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Translation initiation factor eIF4E forms eIF4E-eIF4G complex at the 5’ cap of mRNA. This interaction can be inhibited by the family of 4E-binding proteins (4E-BP). In yeast Saccharomyces cerevisiae, two 4E-BPs, Caf20 and Eap1, compete with eIF4G for binding to eIF4E via the shared conserved interaction motif. In order to investigate the roles of Caf20 in gene-specific translational regulation and the formation of mRNA granules (P-bodies), we introduced substitution mutations, caf20-Y4A or caf20-L9A, in the eIF4E-binding motif for CAF20. Overexpression of the wild-type CAF20 showed an increased protein level of Ste12 transcription factor as well as highly developed P-body formation. However, 4E-binding site mutations of CAF20 led to a reduced number of P-body foci and decreased levels of Ste12 protein. The phenotypes of the caf20 deletion mutation were also analyzed, and we suggest that Caf20 plays a critical role in Ste12 protein expression and in the control of P-body formation.

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    Roles of eIF4E-binding protein Caf20 in Ste12 translation and P-body formation in yeast
    J. Microbiol. 2018;56(10):744-747.   Published online August 22, 2018
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