Human IFT52 mutations uncover a novel role for the protein in microtubule 
dynamics and centrosome cohesion

Dupont, Marie Alice; Humbert, Camille; Huber, Celine; Siour, Quentin; Guerrera, Ida Chiara; Jung, Vincent; Christensen , Anni; Pouliet, Aurore; Garfa-Traore, Meriem; Nitschke, Patrick; Injeyan, Marie; Millar, Kathryn; Chitayat, David; Shannon, Patrick; Girisha, Katta Mohan; Shukla, Anju; Mechler, Charlotte; Lorentzen, Esben; Benmerah, Alexandre; Cormier-Daire, Valerie; Jeanpierre, Cecile; Saunier, Sophie; Delous, Marion

doi:10.1093/hmg/ddz091

Lokale TagsFreigabegeschichteDetailsÜbersicht

Human IFT52 mutations uncover a novel role for the protein in microtubule dynamics and centrosome cohesion

Dupont, M. A., Humbert, C., Huber, C., Siour, Q., Guerrera, I. C., Jung, V., et al. (2019). Human IFT52 mutations uncover a novel role for the protein in microtubule dynamics and centrosome cohesion. HUMAN MOLECULAR GENETICS, 28(16), 2720-2737. doi:10.1093/hmg/ddz091.

Item is Freigegeben

einblenden: alle ausblenden: alle

Basisdaten

einblenden: ausblenden:

Datensatz-Permalink: https://hdl.handle.net/21.11116/0000-0005-8857-0 Versions-Permalink: https://hdl.handle.net/21.11116/0000-0005-8858-F

Genre: Zeitschriftenartikel

ausblenden:

Urheber:
Dupont, Marie Alice¹, Autor
Humbert, Camille¹, Autor
Huber, Celine¹, Autor
Siour, Quentin¹, Autor
Guerrera, Ida Chiara¹, Autor
Jung, Vincent¹, Autor
Christensen , Anni¹, Autor
Pouliet, Aurore¹, Autor
Garfa-Traore, Meriem¹, Autor
Nitschke, Patrick¹, Autor
Injeyan, Marie¹, Autor
Millar, Kathryn¹, Autor
Chitayat, David¹, Autor
Shannon, Patrick¹, Autor
Girisha, Katta Mohan¹, Autor
Shukla, Anju¹, Autor
Mechler, Charlotte¹, Autor
Lorentzen, Esben², Autor
Benmerah, Alexandre¹, Autor
Cormier-Daire, Valerie¹, Autor
Jeanpierre, Cecile¹, AutorSaunier, Sophie¹, AutorDelous, Marion¹, Autor mehr..

Affiliations:
1external, ou_persistent22
2Lorentzen, Esben / Intraflagellar Transport, Max Planck Institute of Biochemistry, Max Planck Society, ou_1565157

Inhalt

einblenden:

ausblenden:

Schlagwörter: INTRAFLAGELLAR TRANSPORT PROTEIN; B CORE; ZEBRAFISH; GENES; CILIA; NEPHRONOPHTHISIS; ALLELES; CANDIDATE; DEFECTS; ENCODESBiochemistry & Molecular Biology; Genetics & Heredity;

Zusammenfassung: Mutations in genes encoding components of the intraflagellar transport (IFT) complexes have previously been associated with a spectrum of diseases collectively termed ciliopathies. Ciliopathies relate to defects in the formation or function of the cilium, a sensory or motile organelle present on the surface of most cell types. IFT52 is a key component of the IFT-B complex and ensures the interaction of the two subcomplexes, IFT-B1 and IFT-B2. Here, we report novel IFT52 biallelic mutations in cases with a short-rib thoracic dysplasia (SRTD) or a congenital anomaly of kidney and urinary tract (CAKUT). Combining in vitro and in vivo studies in zebrafish, we showed that SRTD-associated missense mutation impairs IFT-B complex assembly and IFT-B2 ciliary localization, resulting in decreased cilia length. In comparison, CAKUT-associated missense mutation has a mild pathogenicity, thus explaining the lack of skeletal defects in CAKUT case. In parallel, we demonstrated that the previously reported homozygous nonsense IFT52 mutation associated with Sensenbrenner syndrome [Girisha et al. (2016) A homozygous nonsense variant in IFT52 is associated with a human skeletal ciliopathy. Clin. Genet., 90, 536-539] leads to exon skipping and results in a partially functional protein. Finally, our work uncovered a novel role for IFT52 in microtubule network regulation. We showed that IFT52 interacts and partially co-localized with centrin at the distal end of centrioles where it is involved in its recruitment and/or maintenance. Alteration of this function likely contributes to centriole splitting observed in Ift52(-/-) cells. Altogether, our findings allow a better comprehensive genotype-phenotype correlation among IFT52-related cases and revealed a novel, extra-ciliary role for IFT52, i.e. disruption may contribute to pathophysiological mechanisms.

Details

einblenden:

ausblenden:

Sprache(n): eng - English

Datum: Erschienen: 2019

Publikationsstatus: Erschienen

Seiten: 18

Ort, Verlag, Ausgabe: -

Inhaltsverzeichnis: -

Art der Begutachtung: -

Identifikatoren: ISI: 000493063400008
DOI: 10.1093/hmg/ddz091

Art des Abschluß: -

Veranstaltung

einblenden:

Entscheidung

einblenden:

Projektinformation

einblenden:

Quelle 1

einblenden:

ausblenden:

Titel: HUMAN MOLECULAR GENETICS

Genre der Quelle: Zeitschrift

Urheber:

Affiliations:

Ort, Verlag, Ausgabe: GREAT CLARENDON ST, OXFORD OX2 6DP, ENGLAND : OXFORD UNIV PRESS

Seiten: - Band / Heft: 28 (16) Artikelnummer: - Start- / Endseite: 2720 - 2737 Identifikator: ISSN: 0964-6906

Datensatz

Basisdaten

Dateien

Externe Referenzen

Urheber

Inhalt

Details

Veranstaltung

Entscheidung

Projektinformation

Quelle 1