UBR4/POE facilitates secretory trafficking to maintain circadian clock synchrony

Author:

Hegazi SaraORCID,Cheng Arthur H.ORCID,Krupp Joshua J.ORCID,Tasaki TakafumiORCID,Liu Jiashu,Szulc Daniel A.ORCID,Ling Harrod H.,Rios Garcia Julian,Seecharran ShavanieORCID,Basiri Tayebeh,Amiri Mehdi,Anwar Zobia,Ahmad Safa,Nayal Kamar,Sonenberg Nahum,Liu Bao-Hua,Cheng Hai-Ling MargaretORCID,Levine Joel D.ORCID,Cheng Hai-Ying MaryORCID

Abstract

AbstractUbiquitin ligases control the degradation of core clock proteins to govern the speed and resetting properties of the circadian pacemaker. However, few studies have addressed their potential to regulate other cellular events within clock neurons beyond clock protein turnover. Here, we report that the ubiquitin ligase, UBR4/POE, strengthens the central pacemaker by facilitating neuropeptide trafficking in clock neurons and promoting network synchrony. Ubr4-deficient mice are resistant to jetlag, whereas poe knockdown flies are prone to arrhythmicity, behaviors reflective of the reduced axonal trafficking of circadian neuropeptides. At the cellular level, Ubr4 ablation impairs the export of secreted proteins from the Golgi apparatus by reducing the expression of Coronin 7, which is required for budding of Golgi-derived transport vesicles. In summary, UBR4/POE fulfills a conserved and unexpected role in the vesicular trafficking of neuropeptides, a function that has important implications for circadian clock synchrony and circuit-level signal processing.

Funder

Gouvernement du Canada | Canadian Institutes of Health Research

Gouvernement du Canada | Natural Sciences and Engineering Research Council of Canada

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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