Cilia defects upon loss of WDR4 are linked to proteasomal hyperactivity and ubiquitin shortage-Reference-Cited by-同舟云学术

Cilia defects upon loss of WDR4 are linked to proteasomal hyperactivity and ubiquitin shortage

Published:2024-09-09 Issue:9 Volume:15 Page:
ISSN:2041-4889
Container-title:Cell Death & Disease
language:en
Short-container-title:Cell Death Dis

Author:

Burkhalter Martin D.,Stiff Tom,Maerz Lars D.,Casar Tena Teresa,Wiese Heike,Gerhards Julian,Sailer Steffen A.^ORCID,Vu Linh Anna Trúc,Duong Phu Max,Donow Cornelia,Alupei Marius,Iben Sebastian^ORCID,Groth Marco^ORCID,Wiese Sebastian^ORCID,Church Joseph A.,Jeggo Penelope A.^ORCID,Philipp Melanie^ORCID

Abstract

AbstractThe WD repeat-containing protein 4 (WDR4) has repeatedly been associated with primary microcephaly, a condition of impaired brain and skull growth. Often, faulty centrosomes cause microcephaly, yet aberrant cilia may also be involved. Here, we show using a combination of approaches in human fibroblasts, zebrafish embryos and patient-derived cells that WDR4 facilitates cilium formation. Molecularly, we associated WDR4 loss-of-function with increased protein synthesis and concomitant upregulation of proteasomal activity, while ubiquitin precursor pools are reduced. Inhibition of proteasomal activity as well as supplementation with free ubiquitin restored normal ciliogenesis. Proteasome inhibition ameliorated microcephaly phenotypes. Thus, we propose that WDR4 loss-of-function impairs head growth and neurogenesis via aberrant cilia formation, initially caused by disturbed protein and ubiquitin homeostasis.

Funder

Deutsche Forschungsgemeinschaft

Publisher

Springer Science and Business Media LLC

Link

https://www.nature.com/articles/s41419-024-07042-5.pdf

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