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Transcriptional Networks Controlling the Cell Cycle
Author(s) -
Martin Bonke,
Mikko Turunen,
Maria Sokolova,
Anna Vähärautio,
Teemu Kivioja,
Minna Taipale,
Mikael Björklund,
Jussi Taipale
Publication year - 2013
Publication title -
g3 genes genomes genetics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.468
H-Index - 66
ISSN - 2160-1836
DOI - 10.1534/g3.112.004283
Subject(s) - cyclin dependent kinase 1 , biology , microbiology and biotechnology , mitosis , cell cycle , gene , ribosome , cell division , rna interference , transcriptional regulation , protein biosynthesis , translation (biology) , genetics , cell , gene expression , computational biology , rna , messenger rna
In this work, we map the transcriptional targets of 107 previously identified Drosophila genes whose loss caused the strongest cell-cycle phenotypes in a genome-wide RNA interference screen and mine the resulting data computationally. Besides confirming existing knowledge, the analysis revealed several regulatory systems, among which were two highly-specific and interconnected feedback circuits, one between the ribosome and the proteasome that controls overall protein homeostasis, and the other between the ribosome and Myc/Max that regulates the protein synthesis capacity of cells. We also identified a set of genes that alter the timing of mitosis without affecting gene expression, indicating that the cyclic transcriptional program that produces the components required for cell division can be partially uncoupled from the cell division process itself. These genes all have a function in a pathway that regulates the phosphorylation state of Cdk1. We provide evidence showing that this pathway is involved in regulation of cell size, indicating that a Cdk1-regulated cell size checkpoint exists in metazoans.

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