Rb and FZR1/Cdh1 determine CDK4/6-cyclin D requirement in C. elegans and human cancer cells

Publication date

2015

Authors

The, IngeISNI 0000000393680553
Ruijtenberg, S.A.ISNI 0000000397050268
Bouchet, Benjamin P.ISNI 0000000436377512
Cristobal Gonzalez de Durana, A.ISNI 0000000387577365
Prinsen, Martine B W
van Mourik, TimISNI 000000038955639X
Koreth, John
Xu, Huihong
Heck, AlbertORCID 0000-0002-2405-4404ISNI 0000000393921118
Akhmanova, AnnaISNI 0000000390996464

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Abstract

Cyclin-dependent kinases 4 and 6 (CDK4/6) in complex with D-type cyclins promote cell cycle entry. Most human cancers contain overactive CDK4/6-cyclin D, and CDK4/6-specific inhibitors are promising anti-cancer therapeutics. Here, we investigate the critical functions of CDK4/6-cyclin D kinases, starting from an unbiased screen in the nematode Caenorhabditis elegans. We found that simultaneous mutation of lin-35, a retinoblastoma (Rb)-related gene, and fzr-1, an orthologue to the APC/C co-activator Cdh1, completely eliminates the essential requirement of CDK4/6-cyclin D (CDK-4/CYD-1) in C. elegans. CDK-4/CYD-1 phosphorylates specific residues in the LIN-35 Rb spacer domain and FZR-1 amino terminus, resembling inactivating phosphorylations of the human proteins. In human breast cancer cells, simultaneous knockdown of Rb and FZR1 synergistically bypasses cell division arrest induced by the CDK4/6-specific inhibitor PD-0332991. Our data identify FZR1 as a candidate CDK4/6-cyclin D substrate and point to an APC/C(FZR1) activity as an important determinant in response to CDK4/6-inhibitors.

Keywords

SDG 3 - Good Health and Well-being

Citation

The, I, Ruijtenberg, S, Bouchet, B P, Cristobal Gonzalez de Durana, A, Prinsen, M B W, van Mourik, T, Koreth, J, Xu, H, Heck, A J R, Akhmanova, A, Cuppen, E, Boxem, M, Munoz Murillo, A & van den Heuvel, S 2015, 'Rb and FZR1/Cdh1 determine CDK4/6-cyclin D requirement in C. elegans and human cancer cells', Nature Communications [E], vol. 6, pp. 5906. https://doi.org/10.1038/ncomms6906