Your search keyword '"Isabelle Le Ber"' showing total 7 results

1. Corrigendum to: Recommendations to distinguish behavioural variant frontotemporal dementia from psychiatric disorders

Author

Carole Azuar, Sandra Baez, Caroline Dallaire-Théroux, David C. Perry, Mario Masellis, Chiadi U. Onyike, Annemiek Dols, Daniela Galimberti, Olivier Piguet, Harro Seelaar, Richard Levy, Rik Vandenberghe, Peter Pressman, Calvin Trieu, Mario F. Mendez, Howard J. Rosen, Isabelle Le Ber, Elio Scarpini, Janine Diehl-Schmid, Edward D. Huey, Simon Ducharme, Mathieu Vandenbulcke, Florence Pasquier, Michael Hornberger, Bradley F. Boeve, Alexander Santillo, Flora Gossink, Paulo Caramelli, John C. van Swieten, Ramon Landin-Romero, Fiona Kumfor, Dhamidhu Eratne, Robert Laforce, Yolande A.L. Pijnenburg, Emma Devenney, Maria Landqvist Waldö, Wendy Kelso, Manabu Ikeda, Leonardo Cruz de Souza, Dennis Velakoulis, Jan Van den Stock, Alan J. Lerner, John R. Hodges, Ratnavalli Ellajosyula, and Everard G. B. Vijverberg

Subjects

medicine.medical_specialty, business.industry, Medicine, Neurology (clinical), business, medicine.disease, Psychiatry, Frontotemporal dementia

Abstract

The authors apologize for misspelling the last name of the author Ratnavalli Ellajosyula. This has now been corrected.

Published

2020

2. Why do patients with neurodegenerative frontal syndrome fail to answer: ‘In what way are an orange and a banana alike?’

Author

Emmanuelle Volle, Bruno Dubois, Romain Valabregue, Isabelle Le Ber, Béatrice Garcin, Julien Lagarde, Jean-Christophe Corvol, Marie Vidailhet, and Richard Levy

Subjects

Adult, Male, Elementary cognitive task, Concept Formation, Neuropsychological Tests, Cognitive neuroscience, behavioral disciplines and activities, Alzheimer Disease, medicine, Humans, Prospective Studies, Gray Matter, Prefrontal cortex, Anterior cingulate cortex, Brain Diseases, Neurodegenerative Diseases, Cognition, Middle Aged, medicine.disease, Executive functions, Magnetic Resonance Imaging, Frontal Lobe, medicine.anatomical_structure, Frontal lobe, Frontotemporal Dementia, Female, Neurology (clinical), Psychology, Neuroscience, Psychomotor Performance, Frontotemporal dementia, Cognitive psychology

Abstract

Concept formation is the ability to create an abstract link between dissimilar objects or thoughts and is crucial for abstract and creative thinking. This process is related to the integrity of the prefrontal cortex, given the altered performances reported in patients with frontal damage, particularly those suffering from the behavioural variant of frontotemporal dementia. However, the cognitive mechanisms and neural bases of verbal concept formation are not clearly understood. The present study was aimed at addressing the following unresolved issues regarding concept formation in the field of neurology and cognitive neuroscience: (i) Are alterations in concept formation specific to frontotemporal dementia or are they also present in other cortical neurodegenerative disorders such as Alzheimer's disease? (ii) Is impaired performance in concept formation due to cortical lesions specific to frontotemporal dementia or to a cortico-subcortical frontal syndrome? and (iii) What are the cognitive mechanisms and neural bases underlying concept formation? To address these questions, we designed the Verbal Concept Formation Task, an experimental paradigm based on the similarities test. Patients presenting with severe frontal dysfunction (frontotemporal dementia, n = 18, and the Richardson form of progressive supranuclear palsy, n = 21) or with medial temporal pathology (amnestic mild cognitive impairment or Alzheimer's disease, n = 14) and healthy participants (n = 18) were given the Verbal Concept Formation Task and a large battery of neuropsychological tests. In addition, all participants underwent 3D T1-weighted MRI to analyse grey matter volume using voxel-based morphometry. Frontal patients were significantly impaired on the Verbal Concept Formation Task as compared to non-frontal participants (P = 0.00001). Global performance score was positively correlated with scores in cognitive tasks assessing executive functions and with grey matter volume in several areas, mostly in the frontal-basal-ganglion network. Two types of errors were observed in frontal patients. The most frequent was discriminating instead of grouping items ('linking deficit'). Patients also linked items on a concrete instead of an abstract basis ('abstraction deficit'). Linking and abstraction deficits were related to partially different areas: the linking deficit to the dorsal anterior cingulate cortex, right middle frontal gyrus and both inferior parietal lobules and the abstraction deficit to the head of the caudate nuclei and the left superior frontal gyrus. These data suggest that verbal concept formation requires the integrity of the prefrontal-basal-ganglion functional network. In addition, it can be divided into two distinct cognitive processes, which are underlain by two partially different neural networks.

Published

2014

3. Phenotype variability in progranulin mutation carriers: a clinical, neuropsychological, imaging and genetic study

Author

Valérie Hahn-Barma, Bruno Dubois, Jean-Charles Lambert, Dominique Campion, Serge Bakchine, Agnès Camuzat, Christine Van Broeckhoven, Serge Belliard, Michèle Puel, Patrice Verpillat, Eric Guedj, Alexis Brice, Fabienne Clot, Marie-Odile Habert, Isabelle Le Ber, Jacqueline Mikol, Pascal Lejeune, Ftd-Mnd, Julie van der Zee, Mustapha Ghanim, Didier Hannequin, Vincent Deramecourt, Christian Meyrignac, Martine Vercelletto, Anne Rovelet-Lecrux, Florence Pasquier, Lucette Lacomblez, Vincent de La Sayette, Neurologie et thérapeutique expérimentale, Institut National de la Santé et de la Recherche Médicale (INSERM)-IFR70-Université Pierre et Marie Curie - Paris 6 (UPMC), Génétique médicale et fonctionnelle du cancer et des maladies neuropsychiatriques, Université de Rouen Normandie (UNIROUEN), Normandie Université (NU)-Normandie Université (NU)-Institut National de la Santé et de la Recherche Médicale (INSERM), Service de neurologie [Rouen], CHU Rouen, Normandie Université (NU)-Normandie Université (NU), Department of Genetics, University Hospital, Département de neurologie[Lille], Université de Lille, Droit et Santé-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille), Service Central de Biophysique et de Médecine Nucléaire, Hôpital de la Timone [CHU - APHM] (TIMONE), Centre des Maladies Cognitives et Comportementales [Paris], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Neurodegenerative Brain Diseases Group, Department of Molecular Genetics, Flanders Interuniversity Institute for Biotechnology, Antwerpen, Université de Reims Champagne-Ardenne (URCA), Neurologie générale et maladies inflammatoires du système nerveux [Toulouse], Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-CHU Toulouse [Toulouse]-Hôpital Purpan [Toulouse], CHU Toulouse [Toulouse], Fédération des Maladies du Système Nerveux, Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-CHU Pitié-Salpêtrière [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Sorbonne Université (SU), Service de pharmacologie médicale [CHU Pitié-Salpêtrière], CHU Pitié-Salpêtrière [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Service d′Anatomie et de Cytologie Pathologiques [Lariboisiere], Hôpital Lariboisière-Fernand-Widal [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Neuroendocrinologie et physiopathologie neuronale, Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lille, Droit et Santé, Centre Hospitalier Intercommunal, Centre Hospitalier Départemental, Laboratoire de Neuropsychologie, Université de Caen Normandie (UNICAEN), Normandie Université (NU)-Normandie Université (NU)-École pratique des hautes études (EPHE), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Institut National de la Santé et de la Recherche Médicale (INSERM), Service de Neurologie [CHU Caen], Normandie Université (NU)-Normandie Université (NU)-CHU Caen, Normandie Université (NU)-Tumorothèque de Caen Basse-Normandie (TCBN)-Tumorothèque de Caen Basse-Normandie (TCBN), Service de neurologie [Rennes], Université de Rennes 1 (UR1), Université de Rennes (UNIV-RENNES)-Université de Rennes (UNIV-RENNES), Clinique neurologique, Hôpital Laennec, Service de neurologie, Epidémiologie des maladies chroniques : impact des interactions gène environnement sur la santé des populations, Institut Pasteur de Lille, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lille, Droit et Santé, Laboratoire d'Imagerie Fonctionnelle (LIF), Université Pierre et Marie Curie - Paris 6 (UPMC)-IFR14-IFR49-Institut National de la Santé et de la Recherche Médicale (INSERM), Service de médecine nucléaire [CHU Pitié-Salpétrière], Neuro-anatomie fonctionnelle du comportement et de ses troubles, Université Pierre et Marie Curie - Paris 6 (UPMC)-IFR70-Institut National de la Santé et de la Recherche Médicale (INSERM), Centre du Langage et de Neuropsychologie, Service de Génétique Cytogénétique et Embryologie [CHU Pitié-Salpêtrière], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), ANR-06-MRAR-005-01, ANR, Département de neurologie [Lille], Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille), Centre Hospitalier Universitaire de Toulouse (CHU Toulouse), Normandie Université (NU)-Normandie Université (NU)-École Pratique des Hautes Études (EPHE), Université de Rennes (UR), French research Network on FTD/FTD-MND, and Université de Lille-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)

Subjects

Male, Pathology, Neuropsychological Tests, MESH: Epidemiologic Methods, MESH: Aphasia, Primary Progressive, Apraxia, MESH: Magnetic Resonance Imaging, Primary progressive aphasia, Progranulins, MESH: Aged, 80 and over, 0302 clinical medicine, MESH: Motor Neuron Disease, Corticobasal degeneration, Age of Onset, MESH: Brain Mapping, MESH: Heterozygote, Aged, 80 and over, MESH: Aged, Brain Mapping, 0303 health sciences, MESH: Middle Aged, Parkinsonism, Brain, MESH: Neuropsychological Tests, Middle Aged, Magnetic Resonance Imaging, MESH: Dementia, 3. Good health, Phenotype, Disease Progression, Intercellular Signaling Peptides and Proteins, Female, MESH: Disease Progression, [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Psychology, Haploinsufficiency, Frontotemporal dementia, Adult, Heterozygote, medicine.medical_specialty, MESH: Mutation, MESH: Age of Onset, MESH: Phenotype, MESH: Brain, 03 medical and health sciences, medicine, Humans, Dementia, Motor Neuron Disease, MESH: Intercellular Signaling Peptides and Proteins, Aged, 030304 developmental biology, MESH: Humans, Lewy body, MESH: Adult, medicine.disease, MESH: Male, MESH: Cognition Disorders, Aphasia, Primary Progressive, Mutation, Neurology (clinical), Cognition Disorders, Epidemiologic Methods, MESH: Female, 030217 neurology & neurosurgery

Abstract

Frontotemporal dementia (FTD), characterized by behavioural and language disorders, is a clinically, genetically and pathologically heterogeneous group of diseases. The most recently identified of the four known genes is GRN, associated with 17q-linked FTD with ubiquitin-immunoreactive inclusions. GRN was analysed in 502 probands with frontal variant FTD (fvFTD), FTD with motoneuron disease (FTD-MND), primary progressive aphasia (PPA) and corticobasal degeneration syndrome (CBDS). We studied the clinical, neuropsychological and brain perfusion characteristics of mutation carriers. Eighteen mutations, seven novel were found in 24 families including 32 symptomatic mutation carriers. No copy number variation was found. The phenotypes associated with GRN mutations vary greatly: 20/32 (63%) carriers had fvFTD, the other (12/32, 37%) had clinical diagnoses of PPA, CBDS, Lewy body dementia or Alzheimer's disease. Parkinsonism developed in 13/32 (41%), visual hallucinations in 8/32 (25%) and motor apraxia in 5/21 (24%). Constructional disorders were present in 10/21 (48%). Episodic memory disorders were frequent (16/18, 89%), consistent with hippocampal amnestic syndrome in 5/18 (28%). Hypoperfusion was observed in the hippocampus, parietal lobe and posterior cingulate gyrus, as well as the frontotemporal cortices. The frequency of mutations according to phenotype was 5.7% (20/352) in fvFTD, 17.9% (19/106) in familial forms, 4.4% in PPA (3/68), 3.3% in CBDS (1/30). Hallucinations, apraxia and amnestic syndrome may help differentiate GRN mutation carriers from others FTD patients. Variable phenotypes and neuropsychological profiles, as well as brain perfusion profiles associated with GRN mutations may reflect different patterns of neurodegeneration. Since all the mutations cause a progranulin haploinsufficiency, additional factors probably explain the variable clinical presentation of the disease.

Published

2008

4. A non-DM1, non-DM2 multisystem myotonic disorder with frontotemporal dementia: phenotype and suggestive mapping of the DM3 locus to chromosome 15q21-24

Author

Annie Laquerrière, Nicolas Sergeant, Charles Duyckaerts, Thierry Frebourg, Maria Martinez, Guillaume Bassez, Patrick Magnier, Didier Hannequin, Bruno Eymard, Pascale Saugier-Veber, Thierry Maisonobe, G Raux, Isabelle Le Ber, Christine Bétard, André Delacourte, Dominique Campion, and Carol Girard

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Genetic Linkage, Myotonic Disorder, Tau protein, tau Proteins, Biology, Myotonic dystrophy, Proximal myotonic myopathy, Atrophy, medicine, Humans, Dementia, Sex Ratio, Age of Onset, Muscle, Skeletal, Aged, Chromosomes, Human, Pair 15, Muscle Weakness, Myosin Heavy Chains, Chromosome Mapping, RNA-Binding Proteins, Middle Aged, medicine.disease, Myotonia, Magnetic Resonance Imaging, Pedigree, Phenotype, biology.protein, Female, Neurology (clinical), Myotonic Disorders, Frontotemporal dementia

Abstract

The majority of proximal myotonic myopathy syndromes reported so far have been related to the myotonic dystrophy (DM) type 2 (DM2) mutation, an expanded (CCTG)n repeat in the ZNF9 gene. Here, we describe the phenotype and the histological features in muscle and brain of the first large pedigree with a non-myotonic dystrophy type 1 (DM1) non-DM2 multisystem myotonic disorder associated with severe frontotemporal dementia. Thirty individuals from three generations underwent detailed neurological, neuropsychological, electrophysiological, brain imaging and molecular analyses. Ten of them had proximal muscle weakness at onset, clinical/electrical myotonia and DM-type cataracts. The mean age at onset was 46.7 +/- 12.6 years (range: 32-69). Dementia was observed later in the course of the disease. On muscle biopsies, rare nuclear clumps, rimmed vacuoles and small angulated type 1 and type 2 fibres were seen early in the disease. They were replaced by fibrous adipose tissue at later stages. Immunohistochemical analysis of myosin heavy chain isoforms showed no selective fibre type atrophy-both type 1 and type 2 fibres being affected. Cortical atrophy without white matter lesions was seen on brain MRI. A brain single photon emission computed tomography (SPECT) study revealed marked frontotemporal hypoperfusion. Post-mortem examination of the brains of two patients showing prominent frontotemporal spongiosis, neuronal loss and rare neuronal and glial tau inclusions suggested frontotemporal dementia. Western blot analyses of the tau protein showed a triplet of isoforms (60, 64 and 69 kDa) in neocortical areas, and a doublet (64 and 69 kDa) in subcortical areas that distinguish our myotonic disorder from other's myotonic dystrophies. Molecular analyses failed to detect a repeat expansion in the DMPK and ZNF9 genes excluding both DM1 and DM2, whereas a genome-wide linkage analysis strongly suggested a linkage to chromosome 15q21-24. This previously unreported multisystem myotonic disorder including findings resembling DM1, DM2 and frontotemporal dementia provides further evidence of the clinical and genetic heterogeneity of the myotonic dystrophies. We propose to designate this disease myotonic dystrophy type 3, DM3.

Published

2004

5. Cerebellar ataxia with oculomotor apraxia type 1: clinical and genetic studies

Author

Geneviève Demarquay, Christian Tannier, Alexandra Durr, Sophie Rivaud-Péchoux, Marie-Odile Habert, Alexis Brice, Céline Chamayou, Thierry Kuntzer, Gérard Said, Jean-Marie Beis, Isabelle Le Ber, Michel Koenig, François Ochsner, Marc Tardieu, and Maria-Ceu Moreira

Subjects

Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Pediatrics, medicine.medical_specialty, Ataxia, Cerebellar Ataxia, genetic structures, Apraxias, Neuropsychological Tests, Apraxia, Ocular Motility Disorders, Sural Nerve, medicine, Humans, Oculomotor apraxia, Aprataxin, Adult Apraxias/*genetics/pathology/psychology Cerebellar Ataxia/*genetics/pathology/psychology Cognition Disorders/etiology DNA-Binding Proteins/genetics Disease Progression Electrooculography Humans Magnetic Resonance Imaging Male Mutation Neuropsychological Tests Nuclear Proteins/genetics Ocular Motility Disorders/*genetics/pathology/psychology Phenotype Sural Nerve/ultrastructure, Cerebellar ataxia, Nuclear Proteins, Autosomal recessive cerebellar ataxia, Chorea, medicine.disease, Magnetic Resonance Imaging, DNA-Binding Proteins, Electrooculography, Phenotype, Mutation, Disease Progression, Cerebellar atrophy, Neurology (clinical), medicine.symptom, Cognition Disorders, Psychology, Neuroscience

Abstract

Summary Ataxia with ocular motor apraxia type 1 (AOA1) is an autosomal recessive cerebellar ataxia (ARCA) associated with oculomotor apraxia, hypoalbuminaemia and hypercholesterolaemia. The gene APTX, which encodes aprataxin, has been identified recently. We studied a large series of 158 families with non-Friedreich progressive ARCA. We identified 14 patients (nine families) with five different missense or truncating mutations in the aprataxin gene (W279X, A198V, D267G, W279R, IVS5+1), four of which were new. We determined the relative frequency of AOA1 which is 5%. Mutation carriers underwent detailed neurological, neuropsychological, electrophysiological, oculographic and biological examinations, as well as brain imaging. The mean age at onset was 6.8 6 4.8 years (range 2‐18 years). Cerebellar ataxia with cerebellar atrophy on MRI and severe axonal sensorimotor neuropathy were present in all patients. In contrast, oculomotor apraxia (86%), hypoalbuminaemia (83%) and hypercholesterolaemia (75%) were variable. Choreic movements were frequent at onset (79%), but disappeared in the course of the disease in most cases. However, a remarkably severe and persistent choreic phenotype was associated with one of the mutations (A198V). Cognitive impairment was always present. Ocular saccade initiation was normal, but their duration was increased by the succession of multiple hypometric saccades that could clinically be confused with ‘slow saccades’. We emphasize the phenotypic variability over the course of the disease. Cerebellar ataxia and/or chorea predominate at onset, but later on they are often partially masked by severe neuropathy, which is the most typical symptom in young adults. The presence of chorea, sensorimotor neuropathy, oculomotor anomalies, biological abnormalities, cerebellar atrophy on MRI and absence of the Babinski sign can help to distinguish AOA1 from Friedreich’s ataxia on a clinical basis. The frequency of chorea at onset suggests that this diagnosis should also be considered in children with chorea who do not carry the IT15 mutation responsible for Huntington’s disease.

Published

2003

6. Reply: High prevalence ofCHCHD10mutations in patients with frontotemporal dementia from China: Table 1

Author

Patrick Yu-Wai-Man, Alexis Brice, Karine Nguyen, Véronique Paquis-Flucklinger, Sandra Lacas-Gervais, Emmanuelle C. Genin, Anne de Septenville, Jean Pouget, David Moore, Annabelle Chaussenot, Cécile Rouzier, Charlotte Cochaud, Annie Verschueren, Konstantina Fragaki, Françoise Lespinasse, Yusuke Kageyama, Laetitia Berg-Alonso, Gaëlle Augé, Isabelle Le Ber, Sylvie Bannwarth, Hiromi Sesaki, Valérie Serre, and Samira Ait-El-Mkadem

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, High prevalence, business.industry, Disease, medicine.disease, 3. Good health, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Mitochondrial myopathy, Internal medicine, mental disorders, medicine, In patient, Neurology (clinical), Cognitive decline, Amyotrophic lateral sclerosis, business, Neuroscience, Motor neuropathy, 030217 neurology & neurosurgery, Frontotemporal dementia

Abstract

Sir, In 2014, we provided a genetic basis to support the conclusion that mitochondrial dysfunction can have a causative effect in motor neuron degeneration. We reported a large family with a mitochondrial myopathy associated with motor neuron disease and cognitive decline looking like frontotemporal dementia (FTD). Since the identification of the p.Ser59Leu mutation in the CHCHD10 gene in this family, more than a dozen publications have reported CHCHD10 variants in patient cohorts from different geographic origins. CHCHD10 -related clinical spectrum is continuously expanding and includes FTD, familial or sporadic amyotrophic lateral sclerosis (ALS), FTD-ALS, late-onset spinal motor neuropathy and Charcot-Marie-Tooth disease type 2 (Bannwarth et al. , 2014; Chaussenot et al. , 2014; Johnson et al. , 2014; Muller et al. , 2014; Auranen et al. , 2015; Chio et al. , 2015; Dols-Icardo et al. , 2015; Kurzwelly et al. , 2015; Penttila et al. , 2015; Ronchi et al. , 2015; Zhang et al. , 2015). We read with interest the Letter to the Editor from Bin et al. (2015) suggesting that CHCHD10 is the most important gene linked to FTD in the Chinese population. Among a cohort of 165 patients with ALS and 65 patients with FTD, they identified …

Published

2015

7. Reply: A distinct clinical phenotype in a German kindred with motor neuron disease carrying aCHCHD10mutation: Table 1

Author

Françoise Lespinasse, Cécile Rouzier, Charlotte Cochaud, Emmanuelle C. Genin, Hiromi Sesaki, Patrick Yu-Wai-Man, Annie Verschueren, Konstantina Fragaki, Samira Ait-El-Mkadem, Anne de Septenville, Sylvie Bannwarth, Yusuke Kageyama, Gaëlle Augé, Isabelle Le Ber, Alexis Brice, Valérie Serre, David Moore, Karine Nguyen, Laetitia Berg-Alonso, Véronique Paquis-Flucklinger, Sandra Lacas-Gervais, Jean Pouget, and Annabelle Chaussenot

Subjects

Genetics, 0303 health sciences, Mutation, Disease, Motor neuron, Biology, medicine.disease_cause, medicine.disease, language.human_language, German, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, medicine, language, Neurology (clinical), Amyotrophic lateral sclerosis, Clinical phenotype, 030217 neurology & neurosurgery, 030304 developmental biology, Frontotemporal dementia, Heterozygous mutation

Abstract

Sir, In a relatively short period of time, an increasing body of evidence has accumulated confirming the primary role of mitochondrial dysfunction in frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS) clinical spectrum through the involvement of CHCHD10 both in familial and sporadic cases (Bannwarth et al. , 2014; Chaussenot et al. , 2014; Johnson et al. , 2014; Muller et al. , 2014; Ronchi et al. , 2015). In a new Letter to the Editor submitted to Brain , Kurzwelly et al. (2015) report another large German family with a history of autosomal dominant pure ALS. Affected individuals harboured the c.44G > T (p.Arg15Leu) heterozygous mutation in CHCHD10 , which has been previously identified in five of six families with pure ALS associated with mutations in this gene (two from Germany and three from the USA) (Johnson et al. , 2014; Muller et al. , 2014). The main characteristics of patients reported with CHCHD10 mutations and FTD-ALS clinical spectrum have been summarized in Table 1. The additional German family reported by Kurzwelly et al. highlights several important clinical points that …

Published

2015