Detailed Analysis of ITPR1 Missense Variants Guides Diagnostics and Therapeutic Design

Jussi Pekka Tolonen; Ricardo Parolin Schnekenberg; Simon McGowan; David Sims; Meriel McEntagart; Frances Elmslie; Debbie Shears; Helen Stewart; George K Tofaris; Tabib Dabir; Patrick J Morrison; Diana Johnson; Marios Hadjivassiliou; Sian Ellard; Charles Shaw-Smith; Anna Znaczko; Abhijit Dixit; Mohnish Suri; Ajoy Sarkar; Rachel E Harrison; Gabriela Jones; Henry Houlden; Giorgia Ceravolo; Joanna Jarvis; Jonathan Williams; Morag E Shanks; Penny Clouston; Julia Rankin; Lubov Blumkin; Tally Lerman-Sagie; Penina Ponger; Salmo Raskin; Katariina Granath; Johanna Uusimaa; Hector Conti; Emma McCann; Shelagh Joss; Alexander J M Blakes; Kay Metcalfe; Helen Kingston; Marta Bertoli; Rachel Kneen; Sally Ann Lynch; Inmaculada Martínez Albaladejo; Austen Peter Moore; Wendy D Jones; Genomics England Research Consortium; Esther B E Becker; Andrea H Németh

doi:10.1002/mds.29651

Detailed Analysis of ITPR1 Missense Variants Guides Diagnostics and Therapeutic Design

Mov Disord. 2024 Jan;39(1):141-151. doi: 10.1002/mds.29651. Epub 2023 Nov 14.

Authors

Jussi Pekka Tolonen^{1

2}, Ricardo Parolin Schnekenberg^{1

3}, Simon McGowan⁴, David Sims⁴, Meriel McEntagart⁵, Frances Elmslie⁵, Debbie Shears³, Helen Stewart³, George K Tofaris^{1

2}, Tabib Dabir⁶, Patrick J Morrison⁷, Diana Johnson⁸, Marios Hadjivassiliou⁹, Sian Ellard¹⁰, Charles Shaw-Smith¹¹, Anna Znaczko¹¹, Abhijit Dixit¹², Mohnish Suri¹², Ajoy Sarkar¹², Rachel E Harrison¹², Gabriela Jones¹², Henry Houlden¹³, Giorgia Ceravolo^{13

14}, Joanna Jarvis¹⁵, Jonathan Williams¹⁶, Morag E Shanks¹⁶, Penny Clouston¹⁶, Julia Rankin¹⁷, Lubov Blumkin^{18

19}, Tally Lerman-Sagie^{18

20}, Penina Ponger^{18

21}, Salmo Raskin²², Katariina Granath²³, Johanna Uusimaa²³, Hector Conti²⁴, Emma McCann²⁵, Shelagh Joss²⁶, Alexander J M Blakes^{27

28}, Kay Metcalfe^{27

28}, Helen Kingston²⁸, Marta Bertoli²⁹, Rachel Kneen³⁰, Sally Ann Lynch³¹, Inmaculada Martínez Albaladejo³², Austen Peter Moore³³, Wendy D Jones³⁴; Genomics England Research Consortium³⁵; Esther B E Becker^{1

2}, Andrea H Németh^{1

3}

Affiliations

¹ Nuffield Department of Clinical Neurosciences, University of Oxford, Oxford, UK.
² Kavli Institute of Nanoscience Discovery, University of Oxford, Oxford, UK.
³ Oxford Center for Genomic Medicine, Oxford University Hospitals National Health Service Foundation Trust, University of Oxford, Oxford, UK.
⁴ Centre for Computational Biology, MRC Weatherall Institute of Molecular Medicine, University of Oxford, Oxford, UK.
⁵ South West Regional Genetics Service, St. George's University Hospitals, London, UK.
⁶ Northern Ireland Regional Genetics Service, Belfast City Hospital, Belfast, UK.
⁷ Patrick G. Johnston Centre for Cancer Research and Cell Biology, Queen's University Belfast, Belfast, UK.
⁸ Sheffield Clinical Genetics Service, Sheffield Children's NHS Foundation Trust, Sheffield, UK.
⁹ Department of Neurology, Royal Hallamshire Hospital, Sheffield Teaching Hospital NHS Foundation Trust, Sheffield, UK.
¹⁰ Exeter Genomics Laboratory, Royal Devon University Healthcare NHS Foundation Trust, UK.
¹¹ Peninsula Clinical Genetics Service, Royal Devon University Hospital, Royal Devon University Healthcare NHS Foundation Trust, Exeter, UK.
¹² Department of Clinical Genetics, Nottingham University Hospitals NHS Trust, Nottingham, UK.
¹³ Department of Neuromuscular Disorders, UCL Queen Square Institute of Neurology, University College London, London, UK.
¹⁴ Unit of Pediatric Emergency, Department of Adult and Childhood Human Pathology, University Hospital of Messina, Messina, Italy.
¹⁵ Birmingham Women's and Children's NHS Foundation Trust, Birmingham, UK.
¹⁶ Oxford Regional Genetics Laboratory, Churchill Hospital, Oxford University Hospitals NHS Foundation Trust, Oxford, UK.
¹⁷ Department of Clinical Genetics, Royal Devon and Exeter NHS Foundation Trust, Exeter, UK.
¹⁸ Sackler School of Medicine, Tel Aviv University, Tel Aviv, Israel.
¹⁹ Pediatric Movement Disorders Service, Pediatric Neurology Unit, Edith Wolfson Medical Center, Holon, Israel.
²⁰ Magen Center for Rare Diseases-Metabolic, Neurogenetic, Wolfson Medical Center, Holon, Israel.
²¹ Movement Disorders Unit, Department of Neurology, Tel Aviv Sourasky Medical Center, Tel Aviv, Israel.
²² Genetika Centro de Aconselhamento e Laboratório, Curitiba, Brazil.
²³ Research Unit of Clinical Medicine, Medical Research Center, Oulu University Hospital and University of Oulu, Oulu, Finland.
²⁴ All Wales Medical Genomics Service, Wrexham Maelor Hospital, Wrexham, UK.
²⁵ Liverpool Women's Hospital Foundation Trust, Liverpool, UK.
²⁶ West of Scotland Centre for Genomic Medicine, Queen Elizabeth University Hospital, Glasgow, UK.
²⁷ Division of Evolution, Infection and Genomics, School of Biological Sciences, Faculty of Biology, Medicine and Health, University of Manchester, Manchester, UK.
²⁸ Manchester Centre for Genomic Medicine, University of Manchester, St. Mary's Hospital, Manchester Academic Health Science Centre, Manchester, UK.
²⁹ Northern Genetics Service, International Centre for Life, Newcastle upon Tyne, UK.
³⁰ Department of Neurology, Alder Hey Children's NHS Foundation Trust, Liverpool, UK.
³¹ Department of Clinical Genetics, Children's Health Ireland (CHI) at Crumlin, Dublin, Ireland.
³² Neurology in Pediatrics, Hospital Santa Lucía, Murcia, Spain.
³³ The Walton Centre NHS Foundation Trust, Liverpool, UK.
³⁴ North East Thames Regional Genetics Service, Great Ormond Street Hospital for Children, Great Ormond Street NHS Foundation Trust, London, UK.
³⁵ Department of Health & Social Care, London, UK.

Abstract

Background: The ITPR1 gene encodes the inositol 1,4,5-trisphosphate (IP₃ ) receptor type 1 (IP₃ R1), a critical player in cerebellar intracellular calcium signaling. Pathogenic missense variants in ITPR1 cause congenital spinocerebellar ataxia type 29 (SCA29), Gillespie syndrome (GLSP), and severe pontine/cerebellar hypoplasia. The pathophysiological basis of the different phenotypes is poorly understood.

Objectives: We aimed to identify novel SCA29 and GLSP cases to define core phenotypes, describe the spectrum of missense variation across ITPR1, standardize the ITPR1 variant nomenclature, and investigate disease progression in relation to cerebellar atrophy.

Methods: Cases were identified using next-generation sequencing through the Deciphering Developmental Disorders study, the 100,000 Genomes project, and clinical collaborations. ITPR1 alternative splicing in the human cerebellum was investigated by quantitative polymerase chain reaction.

Results: We report the largest, multinational case series of 46 patients with 28 unique ITPR1 missense variants. Variants clustered in functional domains of the protein, especially in the N-terminal IP₃ -binding domain, the carbonic anhydrase 8 (CA8)-binding region, and the C-terminal transmembrane channel domain. Variants outside these domains were of questionable clinical significance. Standardized transcript annotation, based on our ITPR1 transcript expression data, greatly facilitated analysis. Genotype-phenotype associations were highly variable. Importantly, while cerebellar atrophy was common, cerebellar volume loss did not correlate with symptom progression.

Conclusions: This dataset represents the largest cohort of patients with ITPR1 missense variants, expanding the clinical spectrum of SCA29 and GLSP. Standardized transcript annotation is essential for future reporting. Our findings will aid in diagnostic interpretation in the clinic and guide selection of variants for preclinical studies. © 2023 The Authors. Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society.

Keywords: Gillespie syndrome; IP3R1; ITPR1; cerebellum; next-generation sequencing; spinocerebellar ataxia type 29.

MeSH terms

Aniridia*
Atrophy
Carbonic Anhydrases* / genetics
Carbonic Anhydrases* / metabolism
Cerebellar Ataxia* / genetics
Humans
Inositol 1,4,5-Trisphosphate Receptors / chemistry
Inositol 1,4,5-Trisphosphate Receptors / genetics
Inositol 1,4,5-Trisphosphate Receptors / metabolism
Intellectual Disability*
Intracellular Signaling Peptides and Proteins / genetics
Movement Disorders* / complications
Mutation, Missense / genetics
Spinocerebellar Degenerations*

Substances

Inositol 1,4,5-Trisphosphate Receptors
ITPR1 protein, human
CA8 protein, human
Carbonic Anhydrases
Intracellular Signaling Peptides and Proteins

Supplementary concepts

Aniridia cerebellar ataxia mental deficiency
Spinocerebellar Ataxia 29

Abstract

MeSH terms

Substances

Supplementary concepts

Grants and funding