Your search keyword '"H Houlden"' showing total 24 results

1. RFC1 repeat expansions in downbeat nystagmus syndromes: frequency and phenotypic profile.

Author

Pellerin D, Heindl F, Traschütz A, Rujescu D, Hartmann AM, Brais B, Houlden H, Dufke C, Riess O, Haack T, Strupp M, and Synofzik M

Subjects

Humans, Male, Female, Middle Aged, Adult, Aged, DNA Repeat Expansion genetics, Fibroblast Growth Factors genetics, Young Adult, Bilateral Vestibulopathy genetics, Bilateral Vestibulopathy physiopathology, Replication Protein C genetics, Phenotype, Nystagmus, Pathologic genetics

Abstract

Objectives: The cause of downbeat nystagmus (DBN) remains unknown in a substantial number of patients ("idiopathic"), although intronic GAA expansions in FGF14 have recently been shown to account for almost 50% of yet idiopathic cases. Here, we hypothesized that biallelic RFC1 expansions may also represent a recurrent cause of DBN syndrome., Methods: We genotyped the RFC1 repeat and performed in-depth phenotyping in 203 patients with DBN, including 65 patients with idiopathic DBN, 102 patients carrying an FGF14 GAA expansion, and 36 patients with presumed secondary DBN., Results: Biallelic RFC1 AAGGG expansions were identified in 15/65 patients with idiopathic DBN (23%). None of the 102 GAA-FGF14-positive patients, but 2/36 (6%) of patients with presumed secondary DBN carried biallelic RFC1 expansions. The DBN syndrome in RFC1-positive patients was characterized by additional cerebellar impairment in 100% (15/15), bilateral vestibulopathy (BVP) in 100% (15/15), and polyneuropathy in 80% (12/15) of cases. Compared to GAA-FGF14-positive and genetically unexplained patients, RFC1-positive patients had significantly more frequent neuropathic features on examination and BVP. Furthermore, vestibular function, as measured by the video head impulse test, was significantly more impaired in RFC1-positive patients., Discussion: Biallelic RFC1 expansions are a common monogenic cause of DBN syndrome., (© 2024. The Author(s).)

Published

2024

2. Update on leukodystrophies and developing trials.

Author

Ceravolo G, Zhelcheska K, Squadrito V, Pellerin D, Gitto E, Hartley L, and Houlden H

Subjects

Humans, Magnetic Resonance Imaging, Hereditary Central Nervous System Demyelinating Diseases diagnosis, Hereditary Central Nervous System Demyelinating Diseases genetics, Hereditary Central Nervous System Demyelinating Diseases therapy, Demyelinating Diseases, Lysosomal Storage Diseases, White Matter

Abstract

Leukodystrophies are a heterogeneous group of rare genetic disorders primarily affecting the white matter of the central nervous system. These conditions can present a diagnostic challenge, requiring a comprehensive approach that combines clinical evaluation, neuroimaging, metabolic testing, and genetic testing. While MRI is the main tool for diagnosis, advances in molecular diagnostics, particularly whole-exome sequencing, have significantly improved the diagnostic yield. Timely and accurate diagnosis is crucial to guide symptomatic treatment and assess eligibility to participate in clinical trials. Despite no specific cure being available for most leukodystrophies, gene therapy is emerging as a potential treatment avenue, rapidly advancing the therapeutic prospects in leukodystrophies. This review will explore diagnostic and therapeutic strategies for leukodystrophies, with particular emphasis on new trials., (© 2023. The Author(s).)

Published

2024

3. White matter abnormalities in 15 subjects with SPG76.

Author

Alkhalifa A, Chen S, Hasiloglu ZI, Filosto M, Cali E, Houlden H, Sgobbi de Souza P, Alavi A, Goizet C, Stevanin G, Taithe F, Nicita F, Vasco G, Tozza S, Cocozza S, Carboni N, Figus A, Wu J, Basak AN, Brais B, Rouleau G, and La Piana R

Subjects

Humans, Retrospective Studies, Magnetic Resonance Imaging, White Matter diagnostic imaging, White Matter pathology, Spastic Paraplegia, Hereditary diagnostic imaging, Spastic Paraplegia, Hereditary genetics, Paraparesis, Spastic

Abstract

Background and Objectives: Hereditary spastic paraplegias (HSPs) are heterogenous genetic disorders characterized by progressive pyramidal tract involvement. SPG76 is a recently identified form of HSP, caused by biallelic calpain-1 (CAPN1) variants. The most frequently described MRI abnormality in SPG76 is mild cerebellar atrophy and non-specific white matter abnormalities were reported in only one case. Following the identification of prominent white matter abnormalities in a subject with CAPN1 variants, which delayed the diagnosis, we aimed to verify the presence of MRI patterns of white matter involvement specific to this HSP., Methods: We performed a retrospective radiological qualitative analysis of 15 subjects with SPG76 (4 previously unreported) initially screened for white matter involvement. Moreover, we performed quantitative analyses in our proband with available longitudinal studies., Results: We observed bilateral, periventricular white matter involvement in 12 subjects (80%), associated with multifocal subcortical abnormalities in 5 of them (33.3%). Three subjects (20%) presented only multifocal subcortical involvement. Longitudinal quantitative analyses of our proband revealed increase in multifocal white matter lesion count and increased area of periventricular white matter involvement over time., Discussion: SPG76 should be added to the list of HSPs with associated white matter abnormalities. We identified periventricular white matter involvement in subjects with SPG76, variably associated with multifocal subcortical white matter abnormalities. These findings, in the presence of progressive spastic paraparesis, can mislead the diagnostic process towards an acquired white matter disorder., (© 2023. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany.)

Published

2023

4. Inclusion body myositis: from genetics to clinical trials.

Author

Nagy S, Khan A, Machado PM, and Houlden H

Subjects

Humans, Disease Progression, Myositis, Inclusion Body genetics, Myositis, Inclusion Body therapy, Myositis

Abstract

Inclusion body myositis (IBM) belongs to the group of idiopathic inflammatory myopathies and is characterized by a slowly progressive disease course with asymmetric muscle weakness of predominantly the finger flexors and knee extensors. The disease leads to severe disability and most patients lose ambulation due to lack of curative or disease-modifying treatment options. Despite some genes reported to be associated with hereditary IBM (a distinct group of conditions), data on the genetic susceptibility of sporadic IBM are very limited. This review gives an overview of the disease and focuses on the current genetic knowledge and potential therapeutic implications., (© 2022. The Author(s).)

Published

2023

5. A rare cause of monogenic cerebral small vessel disease and stroke: Cathepsin A-related arteriopathy with strokes and leukoencephalopathy (CARASAL).

Author

Budhdeo S, de Paiva ARB, Wade C, Lopes LCG, Della-Ripa B, Davagnanam I, Lucato L, Mummery CJ, Kok F, Houlden H, Werring DJ, and Lynch DS

Subjects

Female, Humans, Male, Cathepsin A genetics, Magnetic Resonance Imaging, Brain Ischemia complications, Brain Ischemia diagnostic imaging, Brain Ischemia genetics, CADASIL complications, CADASIL diagnostic imaging, CADASIL genetics, Cerebral Small Vessel Diseases complications, Cerebral Small Vessel Diseases diagnostic imaging, Cerebral Small Vessel Diseases genetics, Deglutition Disorders, Leukoencephalopathies complications, Leukoencephalopathies diagnostic imaging, Leukoencephalopathies genetics, Stroke complications, Stroke diagnostic imaging, Tinnitus

Abstract

Background: Cathepsin A-related arteriopathy with strokes and leukoencephalopathy (CARASAL) is a rare monogenic cause of cerebral small vessel disease. To date, fewer than 15 patients with CARASAL have been described, all of common European ancestry., Methods: Clinical and imaging phenotypes of two patients are presented. Genetic variants were identified using targeted Sanger and focused exome sequencing, respectively., Results: Both patients carried the same pathogenic p.Arg325Cys mutation in CTSA. One patient of Chinese ethnicity presented with migraine, tinnitus and slowly progressive cognitive impairment with significant cerebral small vessel disease in the absence of typical cardiovascular risk factors. She later suffered an ischaemic stroke. A second patient from Brazil, of Italian ethnicity developed progressive dysphagia and dysarthria in his 50s, he later developed hearing loss and chronic disequilibrium. Magnetic resonance imaging in both cases demonstrated extensive signal change in the deep cerebral white matter, anterior temporal lobes, thalami, internal and external capsules and brainstem., Conclusions: CARASAL should be considered in patients with early onset or severe cerebral small vessel disease, particularly where there are prominent symptoms or signs related to brainstem involvement, such as hearing dysfunction, tinnitus or dysphagia or where there is significant thalamic and brainstem involvement on imaging., (© 2022. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany.)

Published

2022

6. Correction to: DRPLA: understanding the natural history and developing biomarkers to accelerate therapeutic trials in a globally rare repeat expansion disorder.

Author

Chaudhry A, Athanasiou-Fragkouli A, Garcia-Moreno H, Abadias SP, Greenfield J, Shiloh-Malawsky Y, Giunti P, and Houlden H

Published

2021

7. DRPLA: understanding the natural history and developing biomarkers to accelerate therapeutic trials in a globally rare repeat expansion disorder.

Author

Chaudhry A, Anthanasiou-Fragkouli A, and Houlden H

Subjects

Biomarkers, Humans, Rare Diseases, Trinucleotide Repeat Expansion

Abstract

Dentatorubral-pallidoluysian atrophy (DRPLA) is a rare neurodegenerative disorder caused by CAG repeat expansions in the atrophin-1 gene and is inherited in an autosomal dominant fashion. There are currently no disease-modifying treatments available. The broad development of therapies for DRPLA, as well as other similar rare diseases, has hit a roadblock due to the rarity of the condition and the wide global distribution of patients and families, consequently inhibiting biomarker development and therapeutic research. Considering the shifting focus towards diverse populations, widespread genetic testing, rapid advancements in the development of clinical and wet biomarkers for Huntington's disease (HD), and the ongoing clinical trials for antisense oligonucleotide (ASO) therapies, the prospect of developing effective treatments in rare disorders has completely changed. The awareness of the HD ASO program has prompted global collaboration for rare disorders in natural history studies and the development of biomarkers, with the eventual goal of undergoing treatment trials. Here, we discuss DRPLA, which shares similarities with HD, and how in this and other repeat expansion disorders, neurogenetics groups like ours at UCL are gearing up for forthcoming natural history studies to accelerate future ASO treatment trials to hopefully emulate the progress seen in HD., (© 2020. The Author(s).)

Published

2021

8. CANVAS: a late onset ataxia due to biallelic intronic AAGGG expansions.

Author

Dominik N, Galassi Deforie V, Cortese A, and Houlden H

Subjects

Ataxia genetics, Humans, Introns genetics, Replication Protein C genetics, Bilateral Vestibulopathy, Cerebellar Ataxia genetics

Abstract

The ataxias are a group of disorders that manifest with balance, movement, speech and visual problems. They can arise due to dysfunction of the cerebellum, the vestibular system and/or the sensory neurons. Genetic defects are a common cause of chronic ataxia, particularly common are repeat expansions in this group of conditions. Co-occurrence of cerebellar ataxia with neuropathy and vestibular areflexia syndrome has been termed CANVAS. Although CANVAS is a rare syndrome, on discovery of biallelic expansions in the second intron of replication factor C subunit 1 (RFC1) gene, we and others have found the phenotype is broad and RFC1 expansions are a common cause of late-onset progressive ataxia.We aim to provide a review and update on recent developments in CANVAS and populations, where the disorder has been reported. We have also optimised a protocol for RFC1 expansion screening which is described herein and expanded phenotype after analysing late-onset ataxia patients from around the world.

Published

2021

9. An update on MSA: premotor and non-motor features open a window of opportunities for early diagnosis and intervention.

Author

Chelban V, Catereniuc D, Aftene D, Gasnas A, Vichayanrat E, Iodice V, Groppa S, and Houlden H

Subjects

Early Diagnosis, Humans, Cerebellar Ataxia, Multiple System Atrophy diagnosis, Multiple System Atrophy therapy, Parkinsonian Disorders, Pure Autonomic Failure

Abstract

In this review, we describe the wide clinical spectrum of features that can be seen in multiple system atrophy (MSA) with a focus on the premotor phase and the non-motor symptoms providing an up-to-date overview of the current understanding in this fast-growing field. First, we highlight the non-motor features at disease onset when MSA can be indistinguishable from pure autonomic failure or other chronic neurodegenerative conditions. We describe the progression of clinical features to aid the diagnosis of MSA early in the disease course. We go on to describe the levels of diagnostic certainty and we discuss MSA subtypes that do not fit into the current diagnostic criteria, highlighting the complexity of the disease as well as the need for revised diagnostic tools. Second, we describe the pathology, clinical description, and investigations of cardiovascular autonomic failure, urogenital and sexual dysfunction, orthostatic hypotension, and respiratory and REM-sleep behavior disorders, which may precede the motor presentation by months or years. Their presence at presentation, even in the absence of ataxia and parkinsonism, should be regarded as highly suggestive of the premotor phase of MSA. Finally, we discuss how the recognition of the broader spectrum of clinical features of MSA and especially the non-motor features at disease onset represent a window of opportunity for disease-modifying interventions.

Published

2020

10. A novel frameshift deletion in autosomal recessive SBF1-related syndromic neuropathy with necklace fibres.

Author

Gang Q, Bettencourt C, Holton J, Lovejoy C, Chelban V, Oconnor E, Yuan Y, Reilly MM, Hanna M, and Houlden H

Subjects

Adult, Genes, Recessive, Homozygote, Humans, Intracellular Signaling Peptides and Proteins, Male, Pedigree, Phenotype, Exome Sequencing, Charcot-Marie-Tooth Disease genetics, Frameshift Mutation

Abstract

Objective: To identify the genetic cause of complex neuropathy in two siblings from a consanguineous family., Methods: The patients were recruited from our clinic. Muscle biopsy and whole-exome sequencing (WES) were performed. Fibroblasts cell lines from the index patient, unaffected parents, and three normal controls were used for cDNA analysis and western blot., Results: The index patient was a 29-year-old male with clinical phenotype of syndactyly, pes cavus, swallowing difficulties, vision problem, imbalance, and muscle weakness. The sibling had similar, but milder symptoms. Nerve conduction studies and electromyography of both patients suggested sensory-motor axonal neuropathy. Muscle biopsy showed a feature of necklace fibres. WES identified a novel homozygous frameshift deletion (c.5477-5478del; p.1826-1826del) in exon 40 of the SBF1 gene in the two siblings, while both parents and the unaffected sibling were heterozygous carriers. Functional analysis showed a markedly reduced level of MTMR5 protein encoded by SBF1 in the index case. The levels of MTMR5 protein in unaffected parents were similar to those found in controls., Conclusion: A novel homozygous frameshift deletion in SBF1 was identified in this family. Sensory-motor axonal neuropathy and necklace fibres in biopsy were the major features expanding the phenotypic spectrum of SBF1-related recessive syndromic neuropathy.

Published

2020

11. An update on advances in magnetic resonance imaging of multiple system atrophy.

Author

Chelban V, Bocchetta M, Hassanein S, Haridy NA, Houlden H, and Rohrer JD

Subjects

Brain diagnostic imaging, Humans, Neuroimaging methods, Magnetic Resonance Imaging methods, Multiple System Atrophy diagnostic imaging

Abstract

In this review, we describe how different neuroimaging tools have been used to identify novel MSA biomarkers, highlighting their advantages and limitations. First, we describe the main structural MRI changes frequently associated with MSA including the 'hot cross-bun' and 'putaminal rim' signs as well as putaminal, pontine, and middle cerebellar peduncle (MCP) atrophy. We discuss the sensitivity and specificity of different supra- and infratentorial changes in differentiating MSA from other disorders, highlighting those that can improve diagnostic accuracy, including the MCP width and MCP/superior cerebellar peduncle (SCP) ratio on T1-weighted imaging, raised putaminal diffusivity on diffusion-weighted imaging, and increased T2* signal in the putamen, striatum, and substantia nigra on susceptibility-weighted imaging. Second, we focus on recent advances in structural and functional MRI techniques including diffusion tensor imaging (DTI), resting-state functional MRI (fMRI), and arterial spin labelling (ASL) imaging. Finally, we discuss new approaches for MSA research such as multimodal neuroimaging strategies and how such markers may be applied in clinical trials to provide crucial data for accurately selecting patients and to act as secondary outcome measures.

Published

2019

12. Spinocerebellar ataxia: an update.

Author

Sullivan R, Yau WY, O'Connor E, and Houlden H

Subjects

Humans, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias metabolism, Spinocerebellar Ataxias therapy, Spinocerebellar Ataxias diagnosis

Abstract

Spinocerebellar ataxia (SCA) is a heterogeneous group of neurodegenerative ataxic disorders with autosomal dominant inheritance. We aim to provide an update on the recent clinical and scientific progresses in SCA where numerous novel genes have been identified with next-generation sequencing techniques. The main disease mechanisms of these SCAs include toxic RNA gain-of-function, mitochondrial dysfunction, channelopathies, autophagy and transcription dysregulation. Recent studies have also demonstrated the importance of DNA repair pathways in modifying SCA with CAG expansions. In addition, we summarise the latest technological advances in detecting known and novel repeat expansion in SCA. Finally, we discuss the roles of antisense oligonucleotides and RNA-based therapy as potential treatments.

Published

2019

13. Severe axonal neuropathy is a late manifestation of SPG11.

Author

Manole A, Chelban V, Haridy NA, Hamed SA, Berardo A, Reilly MM, and Houlden H

Subjects

Adolescent, Brain physiopathology, DNA Mutational Analysis, Electromyography, Family Health, Female, Humans, Magnetic Resonance Imaging, Neural Conduction, Peripheral Nerves physiopathology, Polyneuropathies genetics, Spastic Paraplegia, Hereditary genetics, Young Adult, Polyneuropathies physiopathology, Proteins genetics, Spastic Paraplegia, Hereditary physiopathology

Abstract

Complex hereditary spastic paraplegia (HSP) is a clinically heterogeneous group of disorders usually inherited in an autosomal recessive manner. In the past, complex recessive spastic paraplegias have been frequently associated with SPG11 mutations but also with defects in SPG15, SPG7 and a handful of other rare genes. Pleiotropy exists in HSP genes, exemplified in the recent association of SPG11 mutations with CMT2. In this study, we performed whole exome sequence analysis and identified two siblings with novel compound heterozygous frameshift SPG11 mutations. The mutations segregated with disease were not present in control databases and analysis of skin fibroblast derived mRNA indicated that the SPG11 truncated mRNA species were not degraded significantly by non-sense mediated mRNA decay. These siblings had severe early-onset spastic paraplegia but later in their disease developed severe axonal neuropathy, neuropathic pain and blue/black foot discolouration likely caused by a combination of the severe neuropathy with autonomic dysfunction and peripheral oedema. We also identified a similar late-onset axonal neuropathy in a Cypriot SPG11 family. Although neuropathy is occasionally present in SPG11, in our SPG11 patients reported here it was particularly severe, highlighting the association of axonal neuropathy with SPG11 and the late manifestation of axonal peripheral nerve damage., Competing Interests: Compliance with ethical standards Conflicts of interest On behalf of all authors, the corresponding author states that there is no conflict of interest. Ethical standard The work was approved by UCLH ethics committee.

Published

2016

14. Heterogeneity in clinical features and disease severity in ataxia-associated SYNE1 mutations.

Author

Wiethoff S, Hersheson J, Bettencourt C, Wood NW, and Houlden H

Subjects

Adult, Aged, Cerebellar Ataxia complications, Cerebellar Ataxia diagnostic imaging, Cerebellar Ataxia ethnology, Cognition Disorders etiology, Cohort Studies, Cytoskeletal Proteins, Female, Genetic Association Studies, Humans, Magnetic Resonance Imaging, Male, Phenotype, Severity of Illness Index, Sri Lanka, Turkey, United Kingdom, Cerebellar Ataxia genetics, Mutation genetics, Nerve Tissue Proteins genetics, Nuclear Proteins genetics, Pedigree

Abstract

The autosomal recessive spinocerebellar ataxias are an exciting field of study, with a growing number of causal genes and an expanding phenotypic spectrum. SYNE1 was originally discovered in 2007 as the causal gene underlying autosomal recessive spinocerebellar ataxia 1, a disease clinically thought to manifest with mainly pure cerebellar ataxia. Since the original report SYNE1 mutations have also been identified in families with motor neuronopathy and arthrogryposis but few families have been screened as the gene is very large at 146 exons in length. We screened 196 recessive and sporadic ataxia patients for mutations in SYNE1 using next generation sequencing in order to assess its frequency and extend the clinicogenetic spectrum. We identified four novel truncating mutations spread throughout the SYNE1 gene from three families living in London that originated from England, Turkey and Sri Lanka. The phenotype was mainly pure cerebellar ataxia in two families, cognitive decline was present in all three families, axonal neuropathy in one family and marked spasticity in the Turkish family, with a range of disease severities. Searching for genotype-phenotype correlations in the SYNE1 gene, defects located near the 3' prime end of the gene are more frequently associated with motor neuron or neuromuscular involvement so far. Our data indicate SYNE1 mutations are not an uncommon cause of recessive ataxia with or without additional clinical features in patients from various ethnicities. The use of next generation sequencing allows the rapid analysis of large genes and will likely reveal more SYNE1 associated cases and further expand genotype-phenotype correlations.

Published

2016

15. Triple trouble: a striking new phenotype or competing genes in a family with hereditary spastic paraplegia.

Author

Chelban V, Lynch DS, Houlden H, and Wood N

Subjects

Adult, Diagnosis, Differential, Family, Humans, Male, Mutation, Pedigree, Phenotype, Skin pathology, Spastic Paraplegia, Hereditary diagnosis, Spastic Paraplegia, Hereditary pathology, Spastin, Adenosine Triphosphatases genetics, Poly(A)-Binding Protein I genetics, Spastic Paraplegia, Hereditary genetics, Spastic Paraplegia, Hereditary physiopathology

Published

2016

16. Absence of HINT1 mutations in a UK and Spanish cohort of patients with inherited neuropathies.

Author

Horga A, Cottenie E, Tomaselli PJ, Rojas-García R, Salvado M, Villarreal-Pérez L, Gamez J, Márquez-Infante C, Houlden H, and Reilly MM

Subjects

Humans, Pedigree, Spain, United Kingdom, Hereditary Sensory and Motor Neuropathy genetics, Mutation Rate, Nerve Tissue Proteins genetics

Abstract

Biallelic mutations in the HINT1 gene were recently identified as the cause of axonal neuropathy with neuromyotonia. It has been suggested that HINT1 mutations may indeed account for 11% of all inherited neuropathies with autosomal recessive inheritance. However, 81% of patients HINT1-related neuropathies reported to date are originally from five European countries and the global prevalence of the disorder is still unknown. In our study, we aimed to determine the frequency of HINT1 mutations by direct sequencing in a cohort of 152 patients with inherited neuropathies from the UK and Spain, where no cases have been described to date. We failed to identify patients with clinical myotonia, neuromyotonia or pathogenic mutations in HINT1. Our results support that HINT1-related neuropathies are not homogeneously distributed among European populations, which may be explained by founder effects. This geographical variability also underlines the importance of considering the ethnic background when screening for mutations in neuropathy-related genes.

Published

2015

17. Charcot-Marie-Tooth disease type 2C and scapuloperoneal muscular atrophy overlap syndrome in a patient with the R232C TRPV4 mutation.

Author

Koutsis G, Lynch D, Manole A, Karadima G, Reilly MM, Houlden H, and Panas M

Subjects

Adult, Charcot-Marie-Tooth Disease physiopathology, Female, Humans, Muscular Dystrophy, Emery-Dreifuss physiopathology, Mutation, Syndrome, Charcot-Marie-Tooth Disease genetics, Muscular Dystrophy, Emery-Dreifuss genetics, TRPV Cation Channels genetics

Published

2015

18. Erratum to: Charcot-Marie-Tooth disease type 2C and scapuloperoneal muscular atrophy overlap syndrome in a patient with the R232C TRPV4 mutation.

Author

Koutsis G, Lynch D, Manole A, Karadima G, Reilly MM, Houlden H, and Panas M

Published

2015

19. A novel HTRA1 exon 2 mutation causes loss of protease activity in a Pakistani CARASIL patient.

Author

Khaleeli Z, Jaunmuktane Z, Beaufort N, Houlden H, Haffner C, Brandner S, Dichgans M, and Werring D

Subjects

Adult, Female, High-Temperature Requirement A Serine Peptidase 1, Humans, Magnetic Resonance Imaging, Pakistan, Alopecia diagnosis, Alopecia genetics, Cerebral Infarction diagnosis, Cerebral Infarction genetics, Exons genetics, Leukoencephalopathies diagnosis, Leukoencephalopathies genetics, Mutation genetics, Peptide Hydrolases metabolism, Serine Endopeptidases genetics, Spinal Diseases diagnosis, Spinal Diseases genetics

Published

2015

20. Exome sequencing expands the mutational spectrum of SPG8 in a family with spasticity responsive to L-DOPA treatment.

Author

Bettencourt C, Morris HR, Singleton AB, Hardy J, and Houlden H

Subjects

Adult, Age of Onset, Amino Acid Sequence, Base Sequence, Child, DNA Mutational Analysis, Exome, Female, Humans, Male, Molecular Sequence Data, Muscle Spasticity drug therapy, Muscle Spasticity genetics, Mutation, Missense, Paraplegia complications, Paraplegia drug therapy, Paraplegia genetics, Pedigree, Spastic Paraplegia, Hereditary complications, Spastic Paraplegia, Hereditary drug therapy, Spastic Paraplegia, Hereditary genetics, Dopamine Agents therapeutic use, Levodopa therapeutic use, Proteins genetics

Published

2013

21. The frequency of spinocerebellar ataxia type 23 in a UK population.

Author

Fawcett K, Mehrabian M, Liu YT, Hamed S, Elahi E, Revesz T, Koutsis G, Herscheson J, Schottlaender L, Wardle M, Morrison PJ, Morris HR, Giunti P, Wood N, and Houlden H

Subjects

Adult, Aged, Aged, 80 and over, Cohort Studies, Female, Humans, Male, Middle Aged, Prevalence, Spinocerebellar Degenerations diagnosis, United Kingdom epidemiology, Enkephalins genetics, Population Surveillance methods, Protein Precursors genetics, Spinocerebellar Degenerations epidemiology, Spinocerebellar Degenerations genetics

Abstract

Spinocerebellar ataxias (SCA) are a genetically heterogeneous group of neurodegenerative diseases characterised by progressive cerebellar ataxia, dysarthria and oculomotor abnormalities. Recently the prodynorphin (PDYN) gene was identified as the cause of SCA23 in four Dutch families displaying progressive gait and limb ataxia. In this study we aimed to assess the frequency of PDYN gene defects and extend the phenotype of SCA23 patients in a UK ataxia series and also in patients from Greece, Egypt and India. We sequenced the coding and flanking intronic regions of the PDYN gene in a total of 852 ataxia patients, of which 356 were sporadic with no family history, 320 had a positive family history, and 176 probands had a positive family history and at least one family member had also been investigated. We also analysed 190 patients with multiple-system atrophy with cerebellar features (MSA-C), a phenocopy of SCA23. We identified a novel putative pathogenic heterozygous missense variant in the PDYN gene in an early onset SCA patient with an unknown family history. This variant was not present in 570 matched British controls. This is the first study to screen for SCA23 in UK patients and confirms that PDYN mutations are a very rare cause of spinocerebellar ataxia, accounting for ~ 0.1 % of ataxia cases but perhaps with a higher frequency in pure cerebellar ataxia. Given the rarity of PDYN mutations, front-line diagnostic evaluation of UK familial and early onset pure spinocerebellar ataxia patients should focus on other known ataxia genes.

Published

2013

22. Clinical variability and L-Dopa responsive Parkinsonism in hereditary spastic paraplegia 11.

Author

Everett CM, Kara E, Maresh KE, and Houlden H

Subjects

Adult, Humans, Male, Parkinsonian Disorders complications, Pedigree, Spastic Paraplegia, Hereditary complications, Levodopa therapeutic use, Parkinsonian Disorders diagnosis, Parkinsonian Disorders drug therapy, Spastic Paraplegia, Hereditary diagnosis, Spastic Paraplegia, Hereditary drug therapy

Published

2012

23. Genetic screening of Greek patients with Huntington’s disease phenocopies identifies an SCA8 expansion.

Author

Koutsis G, Karadima G, Pandraud A, Sweeney MG, Paudel R, Houlden H, Wood NW, and Panas M

Subjects

Adult, Aged, Brain pathology, Female, Greece, Humans, Huntington Disease pathology, Magnetic Resonance Imaging, Male, Middle Aged, Phenotype, Genetic Testing, Huntington Disease genetics, Spinocerebellar Degenerations genetics, Trinucleotide Repeat Expansion genetics

Abstract

Huntington’s disease (HD) is an autosomal dominant disorder characterized by a triad of chorea, psychiatric disturbance and cognitive decline. Around 1% of patients with HD-like symptoms lack the causative HD expansion and are considered HD phenocopies. Genetic diseases that can present as HD phenocopies include HD-like syndromes such as HDL1, HDL2 and HDL4 (SCA17), some spinocerebellar ataxias (SCAs) and dentatorubral-pallidoluysian atrophy (DRPLA). In this study we screened a cohort of 21 Greek patients with HD phenocopy syndromes formutations causing HDL2, SCA17, SCA1, SCA2, SCA3,SCA8, SCA12 and DRPLA. Fifteen patients (71%) had a positive family history. We identified one patient (4.8% of the total cohort) with an expansion of 81 combined CTA/CTG repeats at the SCA8 locus. This falls within what is believed to be the high-penetrance allele range. In addition to the classic HD triad, the patient had features of dystonia and oculomotor apraxia. There were no cases of HDL2, SCA17, SCA1, SCA2, SCA3, SCA12 or DRPLA. Given the controversy surrounding the SCA8 expansion, the present finding may be incidental. However, if pathogenic, it broadens the phenotype that may be associated with SCA8 expansions. The absence of any other mutations in our cohort is not surprising, given the low probability of reaching a genetic diagnosis in HD phenocopy patients.

Published

2012

24. Frequency of mutations in the genes associated with hereditary sensory and autonomic neuropathy in a UK cohort.

Author

Davidson G, Murphy S, Polke J, Laura M, Salih M, Muntoni F, Blake J, Brandner S, Davies N, Horvath R, Price S, Donaghy M, Roberts M, Foulds N, Ramdharry G, Soler D, Lunn M, Manji H, Davis M, Houlden H, and Reilly M

Subjects

Adolescent, Adult, Child, Child, Preschool, Cohort Studies, Female, Hereditary Sensory and Autonomic Neuropathies epidemiology, Humans, Infant, Newborn, Male, Middle Aged, Pedigree, United Kingdom epidemiology, Young Adult, Hereditary Sensory and Autonomic Neuropathies diagnosis, Hereditary Sensory and Autonomic Neuropathies genetics, Mutation Rate, Serine C-Palmitoyltransferase genetics

Abstract

The hereditary sensory and autonomic neuropathies (HSAN, also known as the hereditary sensory neuropathies) are a clinically and genetically heterogeneous group of disorders, characterised by a progressive sensory neuropathy often complicated by ulcers and amputations, with variable motor and autonomic involvement. To date, mutations in twelve genes have been identified as causing HSAN. To study the frequency of mutations in these genes and the associated phenotypes, we screened 140 index patients in our inherited neuropathy cohort with a clinical diagnosis of HSAN for mutations in the coding regions of SPTLC1, RAB7, WNK1/HSN2, FAM134B, NTRK1 (TRKA) and NGFB. We identified 25 index patients with mutations in six genes associated with HSAN (SPTLC1, RAB7, WNK1/HSN2, FAM134B, NTRK1 and NGFB); 20 of which appear to be pathogenic giving an overall mutation frequency of 14.3%. Mutations in the known genes for HSAN are rare suggesting that further HSAN genes are yet to be identified. The p.Cys133Trp mutation in SPTLC1 is the most common cause of HSAN in the UK population and should be screened first in all patients with sporadic or autosomal dominant HSAN.

Published

2012