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Preservation of circadian rhythms by the protein folding chaperone, BiP.

Citation
Pickard, A., et al. “Preservation Of Circadian Rhythms By The Protein Folding Chaperone, Bip.”. Faseb Journal : Official Publication Of The Federation Of American Societies For Experimental Biology, pp. 7479-7489.
Center University of Michigan
Author Adam Pickard, Joan Chang, Nissrin Alachkar, Ben Calverley, Richa Garva, Peter Arvan, Qing-Jun Meng, Karl E Kadler
Keywords 4PBA, ER stress, Per2::luc, UDCA, Collagen
Abstract

Dysregulation of collagen synthesis is associated with disease progression in cancer and fibrosis. Collagen synthesis is coordinated with the circadian clock, which in cancer cells is, curiously, deregulated by endoplasmic reticulum (ER) stress. We hypothesized interplay between circadian rhythm, collagen synthesis, and ER stress in normal cells. Here we show that fibroblasts with ER stress lack circadian rhythms in gene expression upon clock-synchronizing time cues. Overexpression of binding immunoglobulin protein (BiP) or treatment with chemical chaperones strengthens the oscillation amplitude of circadian rhythms. The significance of these findings was explored in tendon, where we showed that BiP expression is ramped preemptively prior to a surge in collagen synthesis at night, thereby preventing protein misfolding and ER stress. In turn, this forestalls activation of the unfolded protein response in order for circadian rhythms to be maintained. Thus, targeting ER stress could be used to modulate circadian rhythm and restore collagen homeostasis in disease.-Pickard, A., Chang, J., Alachkar, N., Calverley, B., Garva, R., Arvan, P., Meng, Q.-J., Kadler, K. E. Preservation of circadian rhythms by the protein folding chaperone, BiP.

Year of Publication
2019
Journal
FASEB journal : official publication of the Federation of American Societies for Experimental Biology
Volume
33
Issue
6
Number of Pages
7479-7489
Date Published
12/2019
ISSN Number
1530-6860
DOI
10.1096/fj.201802366RR
Alternate Journal
FASEB J.
PMID
30888851
PMCID
PMC6529331
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