Hydrolethalus syndrome (HLS) is a lethal, autosomal recessive ciliopathy caused by the mutation of the conserved centriole protein HYLS1. How HYLS1 controls centriole function is poorly understood. Here, we show that mice harboring the HYLS1 disease mutation die shortly after birth and exhibit developmental defects that recapitulate several manifestations of HLS. These phenotypes arise from a loss of centriole integrity that causes tissue-specific defects in cilia assembly and function. We show that HYLS1 is recruited to the centriole by CEP120 and stabilizes the localization of centriole inner scaffold proteins that ensure the integrity of the centriolar microtubule wall. The HLS disease mutation reduced the centriole localization of HYLS1 and caused degeneration of the centriole distal end. We propose that tissue-specific defects in centriole integrity caused by the HYLS1 mutation prevent ciliogenesis and contribute to HLS phenotypes.
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February 26 2025
Centriole structural integrity defects are a crucial feature of hydrolethalus syndrome
Ana Curinha
,
(Conceptualization, Data curation, Formal analysis, Investigation, Methodology, Project administration, Resources, Supervision, Validation, Visualization, Writing - original draft, Writing - review & editing)
1Department of Molecular Biology and Genetics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Ana Curinha: [email protected]
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Zhaoyu Huang
,
Zhaoyu Huang
*
(Data curation, Formal analysis, Investigation, Validation)
1Department of Molecular Biology and Genetics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
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Taylor Anglen
,
Taylor Anglen
*
(Conceptualization, Investigation, Methodology, Writing - review & editing)
2Department of Biomedical Engineering,
Duke University
, Durham, NC, USA
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Margaret A. Strong
,
Margaret A. Strong
(Investigation, Resources)
1Department of Molecular Biology and Genetics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
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Colin R. Gliech
,
Colin R. Gliech
(Formal analysis, Software, Visualization, Writing - review & editing)
3Department of Rheumatology,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
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Cayla E. Jewett
,
Cayla E. Jewett
(Formal analysis, Investigation, Visualization)
1Department of Molecular Biology and Genetics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
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Anoek Friskes
,
Anoek Friskes
(Investigation)
4Division of Cell Biology,
Oncode Institute, The Netherlands Cancer Institute
, Amsterdam, Netherlands
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Thao P. Phan
,
Thao P. Phan
(Investigation, Methodology)
5Department of Biochemistry and Biophysics,
Cardiovascular Research Institute, University of California, San Francisco
, San Francisco, CA, USA
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Zachary Nicholas
,
Zachary Nicholas
(Conceptualization, Investigation)
6Department of Neuroscience,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
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Andrew J. Holland
(Conceptualization, Formal analysis, Project administration, Resources, Supervision, Writing - original draft, Writing - review & editing)
1Department of Molecular Biology and Genetics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Correspondence to Andrew J. Holland: [email protected]
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Ana Curinha
Conceptualization, Data curation, Formal analysis, Investigation, Methodology, Project administration, Resources, Supervision, Validation, Visualization, Writing - original draft, Writing - review & editing
1Department of Molecular Biology and Genetics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Zhaoyu Huang
Data curation, Formal analysis, Investigation, Validation
*
1Department of Molecular Biology and Genetics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Taylor Anglen
Conceptualization, Investigation, Methodology, Writing - review & editing
*
2Department of Biomedical Engineering,
Duke University
, Durham, NC, USA
Margaret A. Strong
Investigation, Resources
1Department of Molecular Biology and Genetics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Colin R. Gliech
Formal analysis, Software, Visualization, Writing - review & editing
3Department of Rheumatology,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Cayla E. Jewett
Formal analysis, Investigation, Visualization
1Department of Molecular Biology and Genetics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Anoek Friskes
Investigation
4Division of Cell Biology,
Oncode Institute, The Netherlands Cancer Institute
, Amsterdam, Netherlands
Thao P. Phan
Investigation, Methodology
5Department of Biochemistry and Biophysics,
Cardiovascular Research Institute, University of California, San Francisco
, San Francisco, CA, USA
Zachary Nicholas
Conceptualization, Investigation
6Department of Neuroscience,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Correspondence to Andrew J. Holland: [email protected]
Ana Curinha: [email protected]
*
Z. Huang and T. Anglen contributed equally to this paper.
Disclosures: The authors declare no competing interests exist.
Received:
March 04 2024
Revision Received:
November 16 2024
Accepted:
January 21 2025
Online ISSN: 1540-8140
Print ISSN: 0021-9525
Funding
Funder(s):
National Institutes of Health
- Award Id(s): R01 GM133897,R01 GM114119,R01 CA266199
Funder(s):
Damon Runyon Cancer Research Foundation
- Award Id(s): DRG-2478-22
© 2025 Curinha et al.
2025
Curinha et al.
This article is distributed under the terms as described at https://rupress.org/pages/terms102024/.
J Cell Biol (2025) 224 (4): e202403022.
Article history
Received:
March 04 2024
Revision Received:
November 16 2024
Accepted:
January 21 2025
Citation
Ana Curinha, Zhaoyu Huang, Taylor Anglen, Margaret A. Strong, Colin R. Gliech, Cayla E. Jewett, Anoek Friskes, Thao P. Phan, Zachary Nicholas, Andrew J. Holland; Centriole structural integrity defects are a crucial feature of hydrolethalus syndrome. J Cell Biol 3 April 2025; 224 (4): e202403022. doi: https://doi.org/10.1083/jcb.202403022
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