Pure Cerebellar Ataxia with Homozygous Mutations in the PNPLA6 Gene

Wiethoff, Sarah; Bettencourt, Conceição; Paudel, Reema; Madon, Prochi F.; Liu, Yo‐Tsen; Hersheson, Joshua; Wadia, N. H.; Desai, Joy; Houlden, Henry

doi:10.1007/s12311-016-0769-x

Cited by 28 publications

(17 citation statements)

References 17 publications

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“…11 However, it was not before 2014 that mutations in PNPLA6 were also appreciated as a cause of predominant cerebellar ataxia, 12,13 and it has now been shown that PNPLA6 mutations can even cause pure cerebellar ataxia. 14 In light of these observations of patients with predominant or pure cerebellar disease, the terms “SPG7” and “SPG39” reflect the historical meaning at best — and appear to be misnomers for these patients and phenotypes. The fatty acid 2-hydroxylase gene ( FA2H ) is even part of multiple classification systems.…”

Section: Discovering the Phenotypic And Genetic Spectrum From The Extmentioning

confidence: 99%

Overcoming the divide between ataxias and spastic paraplegias: Shared phenotypes, genes, and pathways

2017

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Autosomal-dominant spinocerebellar ataxias, autosomal-recessive spinocerebellar ataxias, and hereditary spastic paraplegias have traditionally been designated in separate clinicogenetic disease classifications. This classification system still largely frames clinical thinking and genetic workup in clinical practice. Yet, with the advent of next-generation sequencing, phenotypically unbiased studies have revealed the limitations of this classification system. Various genes (eg, SPG7, SYNE1, PNPLA6) traditionally rooted in either the ataxia or hereditary spastic paraplegia classification system have now been shown to cause ataxia on the one end of the disease continuum and hereditary spastic paraplegia on the other. Other genes such as GBA2 and KIF1C were almost simultaneously published as both a hereditary spastic paraplegia and an ataxia gene. The variability and fluidity of observed phenotypes along the ataxia-spasticity spectrum warrants a rethinking of the traditional classification system. We propose to replace this divisive diagnosis-driven ataxia and hereditary spastic paraplegia classification system by a descriptive, unbiased approach of modular phenotyping. This approach is also open to expansion of the phenotype beyond ataxia and spasticity, which often occur as part of broader multisystem neuronal dysfunction. The concept of a continuous ataxia-spasticity disease spectrum is further supported by ataxias and hereditary spastic paraplegias sharing not only overlapping phenotypes and underlying genes, but also common cellular pathways and disease mechanisms. This suggests a shared vulnerability of cerebellar and corticospinal neurons for common pathophysiological processes. It might be this mechanistic overlap that drives their clinical overlap. A mechanistically inspired classification system will help to pave the way for mechanism-based strategies for drug development.

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Section: Discovering the Phenotypic And Genetic Spectrum From The Extmentioning

confidence: 99%

Overcoming the divide between ataxias and spastic paraplegias: Shared phenotypes, genes, and pathways

2017

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“…A homozygous mutation in SLC30A9 , which is involved in intracellular zinc homeostasis, was found in a consanguineous Bedouin family with neurological deterioration progressing into severe intellectual disability, profound ataxia, camptocormia, and oculomotor apraxia [ 109 ]. For the first time ever, a report linked PNPLA6 mutations with pure SCA without chorioretinal dystrophy or hypogonadotropic hypogonadism, constituting another example of phenotype expansion [ 110 ]. The next finding is an example of how dominant and recessive mutations in the same gene can lead to completely different phenotypes.…”

Section: Introduction: Advances In the Field Of Rare Diseases Reachedmentioning

confidence: 99%

NGS Technologies as a Turning Point in Rare Disease Research , Diagnosis and Treatment

Fernández–Marmiesse

Gouveia

Couce

2018

CMC

123

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Approximately 25-50 million Americans, 30 million Europeans, and 8% of the Aus-tralian population have a rare disease. Rare diseases are thus a common problem for clini-cians and account for enormous healthcare costs worldwide due to the difficulty of establish-ing a specific diagnosis. In this article, we review the milestones achieved in our understanding of rare diseases since the emergence of next-generation sequencing (NGS) technologies and analyze how these advances have influenced research and diagnosis. The first half of this review describes how NGS has changed diagnostic workflows and provided an unprecedent-ed, simple way of discovering novel disease-associated genes. We focus particularly on meta-bolic and neurodevelopmental disorders. NGS has enabled cheap and rapid genetic diagnosis, highlighted the relevance of mosaic and de novo mutations, brought to light the wide pheno-typic spectrum of most genes, detected digenic inheritance or the presence of more than one rare disease in the same patient, and paved the way for promising new therapies. In the sec-ond part of the review, we look at the limitations and challenges of NGS, including determina-tion of variant causality, the loss of variants in coding and non-coding regions, and the detec-tion of somatic mosaicism variants and epigenetic mutations, and discuss how these can be overcome in the near future.

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“…Autosomal recessive cerebellar ataxias (ARCAs) are a clinically and genetically heterogeneous group of neurodegenerative disorders often associated with additional non-cerebellar features [ 1 ]. Particular phenotypes can be found within this group, such as Gordon Holmes (GHS) and Boucher-Neuhäuser syndromes (BNS), in which ARCAs appeared associated with hypogonadotropic hypogonadism (HH) [ 1 , 2 ].…”

Section: Introductionmentioning

confidence: 99%

Gordon Holmes syndrome due to compound heterozygosity of two new PNPLA6 variants – A diagnostic challenge

et al. 2019

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BackgroundGordon Holmes syndrome (GHS), characterized by cerebellar ataxia and hypogonadotropic hypogonadism (HH), has been related to recessive mutations in PNPLA6 gene.Aims of the studyDescribe one Portuguese family with GHS due to compound heterozygosity of two new PNPLA6 variants.MethodsReport on the clinical presentation, diagnostic and genetic workup to reach GHS diagnosis.ResultsThe index case presented with slight cognitive impairment and primary amenorrhea, developed at the age of 25 a cerebellar syndrome. Her neurological exam revealed ataxia and mild extrapyramidal syndrome. She was born from non-consanguineous parents and had 8 siblings. Two of her sisters also had history of primary amenorrhea, tremor and ataxia. All 3 were diagnosed with HH and previous FMR1 gene screening on her sisters revealed a 51 CGGs allele. However, 2 normal-sized FMR1 alleles were identified on the proband thus excluding the FXTAS diagnosis in the family. Further PNPLA6 variant screening revealed 2 novel variants in compound heterozygosity [c.2404G > C]; [c.4081C > T], which co-segregated with the disease.ConclusionsThis case shows how incomplete studies can be misleading, increases genetic knowledge of GHS and expands its clinical spectrum. The coexistence of a FMR1 intermediate allele in this family constituted an additional challenge in the etiological investigation.

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Pure Cerebellar Ataxia with Homozygous Mutations in the PNPLA6 Gene

Cited by 28 publications

References 17 publications

Overcoming the divide between ataxias and spastic paraplegias: Shared phenotypes, genes, and pathways

Overcoming the divide between ataxias and spastic paraplegias: Shared phenotypes, genes, and pathways

NGS Technologies as a Turning Point in Rare Disease Research , Diagnosis and Treatment

Gordon Holmes syndrome due to compound heterozygosity of two new PNPLA6 variants – A diagnostic challenge

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