A Restricted Repertoire of De Novo Mutations in ITPR1 Cause Gillespie Syndrome with Evidence for Dominant-Negative Effect | Zendy

Meriel McEntagart | Zendy; Kathleen A. Williamson | Zendy; Jacqueline K. Rainger | Zendy; Ann P. Wheeler | Zendy; Anne Seawright | Zendy; Elfride De Baere | Zendy; Hannah Verdin | Zendy; L. Therese Bergendahl | Zendy; Alan J. Quigley | Zendy; Joe Rainger | Zendy; Abhijit Dixit | Zendy; Ajoy Sarkar | Zendy; Eduardo Laso | Zendy; Rocío SánchezCarpintero | Zendy; Jesús BarrioBarrio | Zendy; Pierre Bitoun | Zendy; Trine Prescott | Zendy; Ruth Riise | Zendy; Shane McKee | Zendy; Jackie Cook | Zendy; Lisa McKie | Zendy; Berten Ceulemans | Zendy; Françoise Meire | Zendy; I. Karen Temple | Zendy; Fabienne Prieur | Zendy; Jonathan Williams | Zendy; Penny Clouston | Zendy; Andrea H. Németh | Zendy; Siddharth Banka | Zendy; Hemant Bengani | Zendy; Mark T. Handley | Zendy; Elisabeth Freyer | Zendy; Allyson Ross | Zendy; Veronica van Heyningen | Zendy; Joseph A. Marsh | Zendy; Frances Elmslie | Zendy; David Fitzpatrick | Zendy

Open Access

A Restricted Repertoire of De Novo Mutations in ITPR1 Cause Gillespie Syndrome with Evidence for Dominant-Negative Effect

Author(s) -

Meriel McEntagart,

Kathleen A. Williamson,

Jacqueline K. Rainger,

Ann P. Wheeler,

Anne Seawright,

Elfride De Baere,

Hannah Verdin,

L. Therese Bergendahl,

Alan J. Quigley,

Joe Rainger,

Abhijit Dixit,

Ajoy Sarkar,

Eduardo Laso,

Rocío SánchezCarpintero,

Jesús BarrioBarrio,

Pierre Bitoun,

Trine Prescott,

Ruth Riise,

Shane McKee,

Jackie Cook,

Lisa McKie,

Berten Ceulemans,

Françoise Meire,

I. Karen Temple,

Fabienne Prieur,

Jonathan Williams,

Penny Clouston,

Andrea H. Németh,

Siddharth Banka,

Hemant Bengani,

Mark T. Handley,

Elisabeth Freyer,

Allyson Ross,

Veronica van Heyningen,

Joseph A. Marsh,

Frances Elmslie,

David Fitzpatrick

Publication year - 2016

Publication title -

the american journal of human genetics

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 6.661

H-Index - 302

eISSN - 1537-6605

pISSN - 0002-9297

DOI - 10.1016/j.ajhg.2016.03.018

Subject(s) - biology , missense mutation , genetics , hypotonia , mutation , null allele , phenotype , gene

Gillespie syndrome (GS) is characterized by bilateral iris hypoplasia, congenital hypotonia, non-progressive ataxia, and progressive cerebellar atrophy. Trio-based exome sequencing identified de novo mutations in ITPR1 in three unrelated individuals with GS recruited to the Deciphering Developmental Disorders study. Whole-exome or targeted sequence analysis identified plausible disease-causing ITPR1 mutations in 10/10 additional GS-affected individuals. These ultra-rare protein-altering variants affected only three residues in ITPR1: Glu2094 missense (one de novo, one co-segregating), Gly2539 missense (five de novo, one inheritance uncertain), and Lys2596 in-frame deletion (four de novo). No clinical or radiological differences were evident between individuals with different mutations. ITPR1 encodes an inositol 1,4,5-triphosphate-responsive calcium channel. The homo-tetrameric structure has been solved by cryoelectron microscopy. Using estimations of the degree of structural change induced by known recessive- and dominant-negative mutations in other disease-associated multimeric channels, we developed a generalizable computational approach to indicate the likely mutational mechanism. This analysis supports a dominant-negative mechanism for GS variants in ITPR1. In GS-derived lymphoblastoid cell lines (LCLs), the proportion of ITPR1-positive cells using immunofluorescence was significantly higher in mutant than control LCLs, consistent with an abnormality of nuclear calcium signaling feedback control. Super-resolution imaging supports the existence of an ITPR1-lined nucleoplasmic reticulum. Mice with Itpr1 heterozygous null mutations showed no major iris defects. Purkinje cells of the cerebellum appear to be the most sensitive to impaired ITPR1 function in humans. Iris hypoplasia is likely to result from either complete loss of ITPR1 activity or structure-specific disruption of multimeric interactions.

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