Spinocerebellar ataxia type 29 due to mutations in ITPR1: a case series and review of this emerging congenital ataxia.

Zambonin, Jessica L; Bellomo, Allison; Ben-Pazi, Hilla; Everman, David B; Frazer, Lee M; Geraghty, Michael T; Harper, Amy D; Jones, Julie R; Kamien, Benjamin; Kernohan, Kristin; Koenig, Mary Kay; Lines, Matthew; Palmer, Elizabeth Emma; Richardson, Randal; Segel, Reeval; Tarnopolsky, Mark; Vanstone, Jason R; Gibbons, Melissa; Collins, Abigail; Fogel, Brent L; Dudding-Byth, Tracy; Boycott, Kym M

Zambonin, Jessica L; Bellomo, Allison; Ben-Pazi, Hilla; Everman, David B; Frazer, Lee M; Geraghty, Michael T; Harper, Amy D; Jones, Julie R; Kamien, Benjamin; Kernohan, Kristin; Koenig, Mary Kay; Lines, Matthew; Palmer, Elizabeth Emma; Richardson, Randal; Segel, Reeval; Tarnopolsky, Mark; Vanstone, Jason R; Gibbons, Melissa; Collins, Abigail; Fogel, Brent L; Dudding-Byth, Tracy; Boycott, Kym M.

Affiliation

Zambonin JL; Department of Genetics, Children's Hospital of Eastern Ontario, Ottawa, ON, Canada. jzambonin@cheo.on.ca.
Bellomo A; Greenwood Genetic Center, Greenwood, SC, USA.
Ben-Pazi H; Pediatric Movement Disorders, Neuropediatric Unit, Shaare Zedek Medical Center, Jerusalem, Israel.
Everman DB; Greenwood Genetic Center, Greenwood, SC, USA.
Frazer LM; Greenwood Genetic Center, Greenwood, SC, USA.
Geraghty MT; Children's Hospital of Eastern Ontario Research Institute, Ottawa, ON, Canada.
Harper AD; Carolinas Healthcare System, Charlotte, NC, USA.
Jones JR; Greenwood Genetic Center, Greenwood, SC, USA.
Kamien B; Hunter Genetics, Newcastle, NSW, Australia.
Kernohan K; Department of Genetics, Children's Hospital of Eastern Ontario, Ottawa, ON, Canada.
Koenig MK; Children's Hospital of Eastern Ontario Research Institute, Ottawa, ON, Canada.
Lines M; University of Texas Health Science Center at Houston, Houston, TX, USA.
Palmer EE; Children's Hospital of Eastern Ontario Research Institute, Ottawa, ON, Canada.
Richardson R; Genetics of Learning Disability (GOLD) Service, Waratah, NSW, Australia.
Segel R; University of New South Wales, Randwick, Sydney, Australia.
Tarnopolsky M; Gillette Children's Specialty Healthcare, St Paul, MN, USA.
Vanstone JR; Shaare Zedek Medical Center and the Hebrew University School of Medicine, Jerusalem, Israel.
Gibbons M; Department of Pediatrics, Division of Neuromuscular and Neurometabolic Diseases, McMaster University Medical Centre, Hamilton, ON, Canada.
Collins A; Children's Hospital of Eastern Ontario Research Institute, Ottawa, ON, Canada.
Fogel BL; Department of Neurology, Children's Hospital Colorado, University of Colorado, Denver, School of Medicine, Aurora, CO, USA.
Dudding-Byth T; Program in Neurogenetics, Departments of Neurology and Human Genetics, David Geffen School of Medicine, University of California Los Angeles, Los Angeles, CA, USA.

Orphanet J Rare Dis ; 12(1): 121, 2017 06 28.

Article in En | MEDLINE | ID: mdl-28659154

ABSTRACT

BACKGROUND: Spinocerebellar ataxia type 29 (SCA29) is an autosomal dominant, non-progressive cerebellar ataxia characterized by infantile-onset hypotonia, gross motor delay and cognitive impairment. Affected individuals exhibit cerebellar dysfunction and often have cerebellar atrophy on neuroimaging. Recently, missense mutations in ITPR1 were determined to be responsible. RESULTS: Clinical information on 21 individuals from 15 unrelated families with ITPR1 mutations was retrospectively collected using standardized questionnaires, including 11 previously unreported singletons and 2 new patients from a previously reported family. We describe the genetic, clinical and neuroimaging features of these patients to further characterize the clinical features of this rare condition and assess for any genotype-phenotype correlation for this disorder. Our cohort consisted of 9 males and 12 females, with ages ranging from 28 months to 49 years. Disease course was non-progressive with infantile-onset hypotonia and delays in motor and speech development. Gait ataxia was present in all individuals and 10 (48%) were not ambulating independently between the ages of 3-12 years of age. Mild-to-moderate cognitive impairment was present in 17 individuals (85%). Cerebellar atrophy developed after initial symptom presentation in 13 individuals (72%) and was not associated with disease progression or worsening functional impairment. We identified 12 different mutations including 6 novel mutations; 10 mutations were missense (with 4 present in >1 individual), 1 a splice site mutation leading to an in-frame insertion and 1 an in-frame deletion. No specific genotype-phenotype correlations were observed within our cohort. CONCLUSIONS: Our findings document significant clinical heterogeneity between individuals with SCA29 in a large cohort of molecularly confirmed cases. Based on the retrospective observed clinical features and disease course, we provide recommendations for management. Further research into the natural history of SCA29 through prospective studies is an important next step in better understanding the condition.

Subject(s)

Inositol 1,4,5-Trisphosphate Receptors/genetics; Spinocerebellar Ataxias/genetics; Adolescent; Adult; Cerebellar Ataxia/genetics; Child; Child, Preschool; Female; Humans; Male; Middle Aged; Mutation/genetics; Retrospective Studies; Young Adult

Key words

Cerebellar atrophy; Clinical management; Congenital non-progressive spinocerebellar ataxia; Human phenotype ontologies; ITPR1; SCA29; Spinocerebellar ataxia type 29

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Spinocerebellar Ataxias / Inositol 1,4,5-Trisphosphate Receptors Type of study: Guideline / Observational_studies / Prognostic_studies / Risk_factors_studies Limits: Adolescent / Adult / Child / Child, preschool / Female / Humans / Male / Middle aged Language: En Journal: Orphanet J Rare Dis Journal subject: MEDICINA Year: 2017 Type: Article Affiliation country: Canada

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