Cytoplasmic interaction with CYCLE promotes the post-translational processing of the circadian CLOCK protein

Maurer, Christian; Hung, Hsiu-Cheng; Weber, Frank

doi:10.1016/j.febslet.2009.04.013

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Volume 583, Issue 10 , Pages 1561-1566, 19 May 2009

Cytoplasmic interaction with CYCLE promotes the post-translational processing of the circadian CLOCK protein

Edited by Ulrike Kutay

Biochemistry Center Heidelberg, University of Heidelberg, Im Neuenheimer Feld 328, 69120 Heidelberg, Germany

Received 13 February 2009; received in revised form 2 April 2009; accepted 3 April 2009. published online 17 April 2009.

Abstract

Post-translational regulation of the transcription factor CLOCK (CLK) is crucial for circadian clock function. The contribution of the hetero-dimerization partner CYCLE (CYC) to the post-translational regulation of CLK is largely unknown. Here we report that Drosophila CLK and CYC proteins not only interact in the nucleus, where they activate circadian transcription, but also in the cytoplasm of Drosophila S2R+ cells. Cytoplasmic CLK accumulates in a hypo-phosphorylated state. Impairment of CYC-binding caused a further reduction in CLK phosphorylation, while over-expression of CYC enhanced the phosphorylation of cytoplasmic CLK towards a hypo-phosphorylated state. CYC also promotes nuclear import of CLK, which is required for hyper-phosphorylation of the CLK protein. Our results indicate a role of CYC in the post-translational regulation of the CLK protein.