Heterozygous <scp><i>PNPT1</i></scp> Variants Cause Spinocerebellar Ataxia Type 25

Barbier, Mathieu; Bahlo, Melanie; Pennisi, Alessandra; Jacoupy, Maxime; Tankard, Rick M.; Ewenczyk, Claire; Davies, Kayli C.; Lino, Patricia; Sauty-Colace, Claire; Rafehi, Haloom; Auger, Nicolas; Ansell, Brendan R E; Stelt, Ivo van der; Howell, Katherine; Coutelier, Marie; Amor, David J.; Mundwiller, Emeline; Guillot‐Noël, Léna; Storey, Elsdon; Gardner, R. J McKinlay; Wallis, Mathew; Brusco, Alfredo; Corti, Olga; Rötig, Agnès; Leventer, Richard J.; Brice, Alexis; Delatycki, Martin B.; Stevanin, Giovanni; Lockhart, Paul J.; Dürr, Alexandra

doi:10.1002/ana.26366

Cited by 10 publications

(16 citation statements)

References 43 publications

(109 reference statements)

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“…Additional findings can include deafness (one patient), psychomotor delay as seen in our proband and scoliosis (three children). In time, patients often lose motor abilities: 2 cases, although still ambulant, were unable run, two required a wheelchair (one since adolescence, one at an unknown age), two a K-walker in childhood [2,3]. Our study confirms that SCA25 can indeed manifest in early childhood (occurring within the first three years of life) and contributes to the understanding of the natural history in pediatric patients.…”

Section: Discussionsupporting

confidence: 62%

“…Similar proportions of patients had childhood and adult onset; however, onset in early childhood (birth to 3 years) was observed in only one case. In the present report we describe a second patient who carried a novel PNPT1 variant and had onset of SCA25 already during toddler age [2]…”

Section: Introductionmentioning

confidence: 83%

“…Childhood onset can be a feature of this disease: to date, including the case presented here, 9 out of 18 SCA25 patients for whom information on the age at onset was available had childhood onset. Their phenotype is very variable (Table 1): age at onset ranges from 17 months to 10 years, with ataxic symptoms varying from mild to severe [2,3].…”

Section: Discussionmentioning

confidence: 99%

“…Among these there is SCA25, a SCA subtype which has only recently been better characterized. Indeed, Barbier et al identified the causal gene for this disease to be PNPT1, the mitochondrial olyribonucleotide nucleotidyltransferase 1, and described the associated clinical phenotype in a cohort of patients [2,3]. PNPT1 encodes for an exoribonuclease (PNPase) located in both the mitochondrial intermembrane space and matrix, involved in RNA import and in prevention of the accumulation of double stranded mtRNA in mitochondria [2].…”

Section: Introductionmentioning

confidence: 99%

“…Indeed, Barbier et al identified the causal gene for this disease to be PNPT1, the mitochondrial olyribonucleotide nucleotidyltransferase 1, and described the associated clinical phenotype in a cohort of patients [2,3]. PNPT1 encodes for an exoribonuclease (PNPase) located in both the mitochondrial intermembrane space and matrix, involved in RNA import and in prevention of the accumulation of double stranded mtRNA in mitochondria [2]. Interestingly, bi-allelic pathogenic variants in PNPT1 have been previously associated with different phenotypes, ranging from non-syndromic hearing loss to multisystem Leigh disease [4,5], with a recessive model of inheritance.…”

Section: Introductionmentioning

confidence: 99%

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A Novel Pathogenic Variant in the SCA25-Related Gene Expanding the Etiology of Early-Onset and Progressive Cerebellar Ataxia in Childhood

Ferrera,

Izzo,

Ghezzi

et al. 2023

Neuropediatrics

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Spinocerebellar ataxias (SCAs) are heterogeneous autosomal dominant progressive ataxic disorders. SCA25 has been linked to PNPT1 pathogenic variants. Although pediatric onset is not unusual, to date only one patient with onset in the first years of life has been reported. This study presents an additional case, wherein symptoms emerged during the toddler phase, accompanied by the identification of a novel PNPT1 variant. The childwas seen at 3 years because of frequent falls. Neurological examination revealed cerebellar signsand psychomotor delay. Brain MRI showed cerebellar atrophy (CA), cerebellar cortex and dentate nuclei hyperintensities. Metabolic and genetic testing was inconclusive. At follow up (age 6), the child had clinically and radiologically worsened; ENG revealed axonal sensory neuropathy. Screening of genes associated with ataxias and mitochondrial disease identified a novel, heterozygous variant in PNPT1, which was probably pathogenic. This variant was also detected in the proband’s mother and maternal grandmother both asymptomatic, which aligns with the previously documented incomplete penetrance of heterozygous PNPT1 variants. Our study confirms that SCA25 can have onset in early-childhood and characterizes natural history in pediatric cases: progressive cerebellar ataxia, sensory neuropathy which manifests during the course of the disease. We report for the first time cerebellar gray matter hyperintensities, suggesting that SCA25 should be included in the differential diagnosis of cerebellar ataxias associated with such brain imaging features. In summary, SCA25 should be considered in the diagnostic workup of early onset pediatric progressive ataxias Additionally, we confirm an incomplete penetrance and highly variable expressivity of PNPT1-associated SCA25.

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Section: Discussionsupporting

confidence: 62%

Section: Introductionmentioning

confidence: 83%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

A Novel Pathogenic Variant in the SCA25-Related Gene Expanding the Etiology of Early-Onset and Progressive Cerebellar Ataxia in Childhood

Ferrera,

Izzo,

Ghezzi

et al. 2023

Neuropediatrics

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Nucleotide metabolism, leukodystrophies, and CNS pathology

Gavazzi,

Gonzalez,

Arnold

et al. 2024

J of Inher Metab Disea

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The balance between a protective and a destructive immune response can be precarious, as exemplified by inborn errors in nucleotide metabolism. This class of inherited disorders, which mimics infection, can result in systemic injury and severe neurologic outcomes. The most common of these disorders is Aicardi Goutières syndrome (AGS). AGS results in a phenotype similar to “TORCH” infections (Toxoplasma gondii, Other [Zika virus (ZIKV), human immunodeficiency virus (HIV)], Rubella virus, human Cytomegalovirus [HCMV], and Herpesviruses), but with sustained inflammation and ongoing potential for complications. AGS was first described in the early 1980s as familial clusters of “TORCH” infections, with severe neurology impairment, microcephaly, and basal ganglia calcifications (Aicardi & Goutières, Ann Neurol, 1984;15:49–54) and was associated with chronic cerebrospinal fluid (CSF) lymphocytosis and elevated type I interferon levels (Goutières et al., Ann Neurol, 1998;44:900–907). Since its first description, the clinical spectrum of AGS has dramatically expanded from the initial cohorts of children with severe impairment to including individuals with average intelligence and mild spastic paraparesis. This broad spectrum of potential clinical manifestations can result in a delayed diagnosis, which families cite as a major stressor. Additionally, a timely diagnosis is increasingly critical with emerging therapies targeting the interferon signaling pathway. Despite the many gains in understanding about AGS, there are still many gaps in our understanding of the cell‐type drivers of pathology and characterization of modifying variables that influence clinical outcomes and achievement of timely diagnosis.

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Genetics of Dominant Ataxias

Stevanin

2023

Contemporary Clinical Neuroscience

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Heterozygous PNPT1 Variants Cause Spinocerebellar Ataxia Type 25

Cited by 10 publications

References 43 publications

A Novel Pathogenic Variant in the SCA25-Related Gene Expanding the Etiology of Early-Onset and Progressive Cerebellar Ataxia in Childhood

A Novel Pathogenic Variant in the SCA25-Related Gene Expanding the Etiology of Early-Onset and Progressive Cerebellar Ataxia in Childhood

Nucleotide metabolism, leukodystrophies, and CNS pathology

Genetics of Dominant Ataxias

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