Your search keyword '"Chabrol, Brigitte"' showing total 28 results

1. Autosomal Dominant MPAN: Mosaicism Expands the Clinical Spectrum to Atypical Late‐Onset Phenotypes.

Author

Angelini, Chloé, Durand, Christelle Marie, Fergelot, Patricia, Deforges, Julie, Vital, Anne, Menegon, Patrice, Sarrazin, Elizabeth, Bellance, Rémi, Mathis, Stéphane, Gonzalez, Victoria, Renaud, Mathilde, Frismand, Solène, Schmitt, Emmanuelle, Rouanet, Marie, Burglen, Lydie, Chabrol, Brigitte, Desnous, Béatrice, Arveiler, Benoît, Stevanin, Giovanni, and Coupry, Isabelle

Abstract

Background: Mitochondrial membrane protein‐associated neurodegeneration (MPAN) is caused by mutations in the C19orf12 gene. MPAN typically appears in the first two decades of life and presents with progressive dystonia‐parkinsonism, lower motor neuron signs, optic atrophy, and abnormal iron deposits predominantly in the basal ganglia. MPAN, initially considered as a strictly autosomal recessive disease (AR), turned out to be also dominantly inherited (AD). Objectives: Our aim was to better characterize the clinical, molecular, and functional spectra associated with such dominant pathogenic heterozygous C19orf12 variants. Methods: We collected clinical, imaging, and molecular information of eight individuals from four AD‐MPAN families and obtained brain neuropathology results for one. Functional studies, focused on energy and iron metabolism, were conducted on fibroblasts from AD‐MPAN patients, AR‐MPAN patients, and controls. Results: We identified four heterozygous C19orf12 variants in eight AD‐MPAN patients. Two of them carrying the familial variant in mosaic displayed an atypical late‐onset phenotype. Fibroblasts from AD‐MPAN showed more severe alterations of iron storage metabolism and autophagy compared to AR‐MPAN cells. Conclusion: Our data add strong evidence of the realness of AD‐MPAN with identification of novel monoallelic C19orf12 variants, including at the mosaic state. This has implications in diagnosis procedures. We also expand the phenotypic spectrum of MPAN to late onset atypical presentations. Finally, we demonstrate for the first time more drastic abnormalities of iron metabolism and autophagy in AD‐MPAN than in AR‐MPAN. © 2023 The Authors. Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society. [ABSTRACT FROM AUTHOR]

Published

2023

2. Very long‐term outcomes in 23 patients with cblA type methylmalonic acidemia.

Author

Marelli, Cecilia, Fouilhoux, Alain, Benoist, Jean‐Francois, De Lonlay, Pascale, Guffon‐Fouilhoux, Nathalie, Brassier, Anais, Cano, Aline, Chabrol, Brigitte, Pennisi, Alessandra, Schiff, Manuel, Acquaviva, Cecile, Murphy, Elaine, Servais, Aude, and Lachmann, Robin

Abstract

Objectives: To present the very long‐term follow up of patients with cobalamin A (cblA) deficiency. Methods: A retrospective case series of adult (>16 years) patients with molecular or enzymatic diagnosis of cblA deficiency. Results: We included 23 patients (mean age: 27 ± 7.6 years; mean follow‐up: 24.9 ± 7.6 years). Disease onset was mostly pediatric (78% < 1 year, median = 4 months) with acute neurologic deterioration (65%). Eight patients presented with chronic symptoms, and one had an adult‐onset mild cblA deficiency. Most of the patients (61%) were initially classified as vitamin B12‐unresponsive methylmalonic aciduria (MMA); in vitro B12 responsiveness was subsequently found in all the tested patients (n = 13). Initial management consisted of protein restriction (57%), B12 (17%), or both (26%). The main long‐term problems were intellectual disability (39%) and renal failure (30%). However, 56.5% of the patients were living independently. Intellectual disability was equally distributed among the initial treatment groups, while renal failure (moderate and beginning at the age of 38 years) was present in only one out of seven patients initially treated with B12. Conclusions: We provide a detailed picture of the long‐term outcome of a series of adult cblA patients, mostly diagnosed before the enzymatic and molecular era. We confirm that about 35% of the patients do not present acutely, underlining the importance of measuring MMA in any case of unexplained chronic renal failure, intellectual disability, or growth delay. In addition, we describe a patient with a milder adult‐onset form. Early B12 supplementation seems to protect from severe renal insufficiency. [ABSTRACT FROM AUTHOR]

Published

2022

3. Motor unit number index: A potential electrophysiological biomarker for pediatric spinal muscular atrophy.

Author

Boulay, Christophe, Delmont, Emilien, Audic, Frédérique, Chabrol, Brigitte, and Attarian, Shahram

Abstract

Introduction/Aims: In adult spinal muscular atrophy (SMA), the motor unit number index (MUNIX) has been shown to be an useful electrophysiological biomarker. This study evaluated the feasibility and the clinical relevance of using the MUNIX technique for patients with pediatric SMA (Ped‐SMA) and correlated MUNIX results with clinical scores. Methods: Fourteen patients with type II Ped‐SMA (11 females; median age 11 y [interquartile range (IQR), 4.8–17 y]) and 14 controls (nine females; median age 10.75 y [IQR, 6.5–13.4 y]) were enrolled and matched by sex, age, height, weight, and body mass index. Clinical examination included manual muscle testing, dynamometry (grasp and pinch), and motor function measure (MFM). The MUNIX technique was evaluated in the abductor digiti minimi (ADM) and abductor pollicis brevis (APB) on two sides when possible. Results: In the patients with Ped‐SMA, the MUNIX and compound muscle action potential (CMAP) amplitudes were significantly decreased and the motor size unit index (MUSIX) was significantly increased in the ADM and APB when compared to controls. The intraclass correlation coefficient was good for the intrarater variability of the CMAP amplitude, MUNIX, and MUSIX in the ADM (0.95, 0.83, and 0.89, respectively) and the APB (0.98, 0.96, and 0.94, respectively). The total CMAP amplitude correlated with the grasp and pinch scores (P <.05), and the MUNIX measurements correlated with the MFM scores. Discussion: The MUNIX technique, which accurately estimated lower motor neuron loss and the number of remaining functional motor units, was shown to be a useful electrophysiological biomarker for disease progression and a potential biomarker for treatment response. [ABSTRACT FROM AUTHOR]

Published

2021

4. Clinical and biological characterization of 20 patients with TANGO2 deficiency indicates novel triggers of metabolic crises and no primary energetic defect.

Author

Bérat, Claire‐Marine, Montealegre, Sebastian, Wiedemann, Arnaud, Nuzum, Malou Le Corronc, Blondel, Amélie, Debruge, Hugo, Cano, Aline, Chabrol, Brigitte, Hoebeke, Célia, Polak, Michel, Stoupa, Athanasia, Feillet, François, Torre, Stéphanie, Boddaert, Nathalie, Bruel, Henri, Barth, Magalie, Damaj, Lena, Abi‐Wardé, Marie‐Thérèse, Afenjar, Alexandra, and Benoist, Jean‐François

Abstract

TANGO2 disease is a severe inherited disorder associating multiple symptoms such as metabolic crises, encephalopathy, cardiac arrhythmias, and hypothyroidism. The mechanism of action of TANGO2 is currently unknown. Here, we describe a cohort of 20 French patients bearing mutations in the TANGO2 gene. We found that the main clinical presentation was the association of neurodevelopmental delay (n = 17), acute metabolic crises (n = 17) and hypothyroidism (n = 12), with a large intrafamilial clinical variability. Metabolic crises included rhabdomyolysis (15/17), neurological symptoms (14/17), and cardiac features (12/17; long QT (n = 10), Brugada pattern (n = 2), cardiac arrhythmia (n = 6)) that required intensive care. We show previously uncharacterized triggers of metabolic crises in TANGO2 patients, such as some anesthetics and possibly l‐carnitine. Unexpectedly, plasma acylcarnitines, plasma FGF‐21, muscle histology, and mitochondrial spectrometry were mostly normal. Moreover, in patients' primary myoblasts, palmitate and glutamine oxidation rates, and the mitochondrial network were also normal. Finally, we found variable mitochondrial respiration and defective clearance of oxidized DNA upon cycles of starvation and refeeding. We conclude that TANGO2 disease is a life‐threatening disease that needs specific cardiac management and anesthesia protocol. Mechanistically, TANGO2 disease is unlikely to originate from a primary mitochondrial defect. Rather, we suggest that mitochondrial defects are secondary to strong extrinsic triggers in TANGO2 deficient patients. [ABSTRACT FROM AUTHOR]

Published

2021

5. Clinical characteristics of paediatric COVID‐19 patients followed for up to 13 months.

Author

Matteudi, Tatiana, Luciani, Léa, Fabre, Alexandre, Minodier, Philippe, Boucekine, Mohammed, Bosdure, Emmanuelle, Dubus, Jean‐Christophe, Colson, Philippe, Chabrol, Brigitte, and Morand, Aurélie

Subjects

COVID-19, CHILD patients, POST-acute COVID-19 syndrome, MULTISYSTEM inflammatory syndrome in children, COUGH

Abstract

Clinical characteristics of paediatric COVID-19 patients followed for up to 13 months Abbreviations SARS-CoV-2 severe acute respiratory syndrome coronavirus 2 INTRODUCTION Children are less affected by COVID-19 than adults.1 But, a small proportion of children develop paediatric inflammatory multisystem syndrome,2 with potentially lethal consequences. Most (83.2%) completely recovered and 16.8% had symptoms of long COVID-19: 10/23 had persistent symptoms and 13/23 had new late-onset symptoms, which appeared long after the acute infection, at a mean of 180 days (range 36-345). [Extracted from the article]

Published

2021

6. Extension of the phenotypic spectrum of GLE1‐related disorders to a mild congenital form resembling congenital myopathy.

Author

Cerino, Mathieu, Di Meglio, Chloé, Albertini, Francesca, Audic, Frédérique, Riccardi, Florence, Boulay, Christophe, Philip, Nicole, Bartoli, Marc, Lévy, Nicolas, Krahn, Martin, and Chabrol, Brigitte

Subjects

CONGENITAL disorders, MOTOR neuron diseases, NEMALINE myopathy, MOTOR neurons, AMYOTROPHIC lateral sclerosis, NEUROMUSCULAR diseases, MUSCLE diseases

Abstract

Background: GLE1 (GLE1, RNA Export Mediator, OMIM#603371) variants are associated with severe autosomal recessive motor neuron diseases, that are lethal congenital contracture syndrome 1 (LCCS1, OMIM#253310) and congenital arthrogryposis with anterior horn cell disease (CAAHD, OMIM#611890). The clinical spectrum of GLE1‐related disorders has been expanding these past years, including with adult‐onset amyotrophic lateral sclerosis (ALS) GLE1‐related forms, especially through the new molecular diagnosis strategies associated with the emergence of next‐generation sequencing (NGS) technologies. However, despite this phenotypic variability, reported congenital or ALS adult‐onset forms remain severe, leading to premature death. Methods: Through multidisciplinary interactions between our Neuropediatric and Medical Genetics departments, we were able to diagnose two siblings presenting with congenital disorder, using an NGS approach accordingly to the novel French national recommendations. Results: Two siblings with very similar clinical features, meaning neuromuscular disorder of neonatal onset with progressive improvement, were examined in our Neuropediatrics department. The clinical presentation evoked initially congenital myopathy with autosomal recessive inheritance. However, additional symptoms such as mild dysmorphic features including high anterior hairline, downslanted palpebral fissures, anteverted nares, smooth philtrum with thin upper‐lip, narrow mouth and microretrognathia or delayed expressive language and postnatal growth retardation were suggestive of a more complex clinical presentation and molecular diagnosis. Our NGS approach revealed an unexpected molecular diagnosis for these two siblings, meaning the presence of the homozygous c.1808G>T GLE1 variant. Conclusions: We here report the mildest phenotype ever described, in two siblings carrying the homozygous c.1808G>T GLE1 variant, further widening the clinical spectrum of GLE1‐related diseases. Moreover, by reflecting current medical practice, this case report confirms the importance of establishing regular multidisciplinary meetings, essential for discussing such difficult clinical presentations to finally enable molecular diagnosis, especially when NGS technologies are used. [ABSTRACT FROM AUTHOR]

Published

2020

7. Bromazepam intoxication in an infant: Contribution of hair and nail analysis.

Author

Pelissier‐Alicot, Anne‐Laure, Kintz, Pascal, Ameline, Alice, Bosdure, Emmanuelle, Chabrol, Brigitte, Neant, Nadège, Torrents, Romain, Sastre, Caroline, Baillif‐Couniou, Valérie, Tuchtan‐Torrents, Lucile, and Leonetti, Georges

Published

2020

8. Clinical features and evolution of juvenile myasthenia gravis in a French cohort.

Author

Barraud, Coline, Desguerre, Isabelle, Barnerias, Christine, Gitiaux, Cyril, Boulay, Christophe, and Chabrol, Brigitte

Subjects

MYASTHENIA gravis treatment, CHOLINERGIC receptors, AGE factors in disease, AUTOANTIBODIES, HOSPITAL care, IMMUNOADSORPTION, INTENSIVE care units, LONGITUDINAL method, MYASTHENIA gravis, TRANSFERASES, DISEASE remission, RETROSPECTIVE studies, DISEASE progression

Abstract

Introduction: In this study we determined the clinical, paraclinical, and treatment-related features of juvenile myasthenia gravis (JMG) as well as the clinical course in a cohort of French children.Methods: We conducted a retrospective study of 40 patients with JMG at 2 French pediatric neurology departments from April 2004 to April 2014.Results: Among the patients, 70% had generalized JMG, 52% had positive acetylcholine receptor antibodies, 8% had muscle-specific kinase antibodies, and 40% were seronegative. Treatment with acetylcholinesterase inhibitors was effective and sufficient in 47% of patients. The 6 patients with generalized JMG treated with rituximab and/or immunoadsorption showed improvement. Thirty percent of the patients required hospitalization in an intensive care unit during follow-up (mean 4.7 years). Remission without treatment occurred in 18% of patients.Discussion: As with adults, JMG has high morbidity, particularly among children with generalized symptoms, and rituximab should be considered early in the course of the disease as a second-line treatment. Muscle Nerve 57: 603-609, 2018. [ABSTRACT FROM AUTHOR]

Published

2018

9. How chromosomal deletions can unmask recessive mutations? Deletions in 10q11.2 associated with CHAT or SLC18A3 mutations lead to congenital myasthenic syndrome.

Author

Schwartz, Mathias, Sternberg, Damien, Whalen, Sandra, Afenjar, Alexandra, Isapof, Arnaud, Chabrol, Brigitte, Portnoï, Marie‐France, Heide, Solveig, Keren, Boris, Chantot‐Bastaraud, Sandra, and Siffroi, Jean‐Pierre

Abstract

A congenital myasthenia was suspected in two unrelated children with very similar phenotypes including several episodes of severe dyspnea. Both children had a 10q11.2 deletion revealed by Single Nucleotide Polymorphisms array or by Next Generation Sequencing analysis. The deletion was inherited from the healthy mother in the first case. These deletions unmasked a recessive mutation at the same locus in both cases, but in two different genes: CHAT and SLC18A3. [ABSTRACT FROM AUTHOR]

Published

2018

10. Neurocognitive profiles in MSUD school-age patients.

Author

Bouchereau, Juliette, Leduc-Leballeur, Julie, Pichard, Samia, Imbard, Apolline, Benoist, Jean-François, Abi Warde, Marie-Thérèse, Arnoux, Jean-Baptiste, Barbier, Valérie, Brassier, Anaïs, Broué, Pierre, Cano, Aline, Chabrol, Brigitte, Damon, Gilles, Gay, Claire, Guillain, Isabelle, Habarou, Florence, Lamireau, Delphine, Ottolenghi, Chris, Paermentier, Laetitia, and Sabourdy, Frédérique

Abstract

Maple syrup urine disease (MSUD), an inborn error of amino acids catabolism is characterized by accumulation of branched chain amino acids (BCAAs) leucine, isoleucine, valine and their corresponding alpha-ketoacids. Impact on the cognitive development has been reported historically, with developmental delays of varying degree. Currently, earlier diagnosis and improved management allow a better neurodevelopment, without requirement of special education. However, specific impairments can be observed, and so far, results of detailed neurocognitive assessments are not available. The aim of this study was to analyse neurocognitive profiles of French MSUD patients. This was a multicentre retrospective study on MSUD patients who underwent neurocognitive evaluation at primary school age. Twenty-one patients with classical neonatal onset MSUD were included. The patients' mean age at the time of evaluation was 8.7 years. The mean intellectual quotient (IQ) score was in the normal range (95.1 ± 12.6). In a subset of eight patients, a consistent developmental pattern of higher verbal than performance IQ was observed (mean of the difference 25.7 ± 8.7, p < 0.0001). No correlation could be established between this pattern and long-term metabolic balance (BCAA blood levels), or severity of acute metabolic imbalances, or leucine blood levels at diagnosis and time to toxin removal procedure. These data show that some MSUD patients may exhibit an abnormal neurocognitive profile with higher verbal than performance abilities. This might suggest an executive dysfunction disorder that would need to be further investigated by specialized testing. This pattern is important to detect in MSUD, as appropriate neuropsychological treatment strategies should be proposed. [ABSTRACT FROM AUTHOR]

Published

2017

11. ALG6-CDG: a recognizable phenotype with epilepsy, proximal muscle weakness, ataxia and behavioral and limb anomalies.

Author

Morava, Eva, Tiemes, Vera, Thiel, Christian, Seta, Nathalie, Lonlay, Pascale, Klerk, Hans, Mulder, Margot, Rubio-Gozalbo, Estela, Visser, Gepke, Hasselt, Peter, Horovitz, Dafne, Souza, Carolina, Schwartz, Ida, Green, Andrew, Al-Owain, Mohammed, Uziel, Graciella, Sigaudy, Sabine, Chabrol, Brigitte, Spronsen, Franc-Jan, and Steinert, Martin

Abstract

Introduction: Alpha-1,3-glucosyltransferase congenital disorder of glycosylation (ALG6-CDG) is a congenital disorder of glycosylation. The original patients were described with hypotonia, developmental disability, epilepsy, and increased bleeding tendency. Methods: Based on Euroglycan database registration, we approached referring clinicians and collected comprehensive data on 41 patients. Results: We found hypotonia and developmental delay in all ALG6-CDG patients and epilepsy, ataxia, proximal muscle weakness, and, in the majority of cases, failure to thrive. Nine patients developed intractable seizures. Coagulation anomalies were present in <50 % of cases, without spontaneous bleedings. Facial dysmorphism was rare, but seven patients showed missing phalanges and brachydactyly. Cyclic behavioral change, with autistic features and depressive episodes, was one of the most significant complaints. Eleven children died before the age of 4 years due to protein losing enteropathy (PLE), sepsis, or seizures. The oldest patient was a 40 year-old Dutch woman. The most common pathogenic protein alterations were p.A333V and p.I299Del, without any clear genotype-phenotype correlation. Discussion: ALG6-CDG has been now described in 89 patients, making it the second most common type of CDG. It has a recognizable phenotype and a primary neurologic presentation. [ABSTRACT FROM AUTHOR]

Published

2016

12. Impact of age at onset and newborn screening on outcome in organic acidurias.

Author

Heringer, Jana, Valayannopoulos, Vassili, Lund, Allan, Wijburg, Frits, Freisinger, Peter, Barić, Ivo, Baumgartner, Matthias, Burgard, Peter, Burlina, Alberto, Chapman, Kimberly, Saladelafont, Elisenda, Karall, Daniela, Mühlhausen, Chris, Riches, Victoria, Schiff, Manuel, Sykut-Cegielska, Jolanta, Walter, John, Zeman, Jiri, Chabrol, Brigitte, and Kölker, Stefan

Abstract

Background and aim: To describe current diagnostic and therapeutic strategies in organic acidurias (OADs) and to evaluate their impact on the disease course allowing harmonisation. Methods: Datasets of 567 OAD patients from the E-IMD registry were analysed. The sample includes patients with methylmalonic (MMA, n = 164), propionic (PA, n = 144) and isovaleric aciduria (IVA, n = 83), and glutaric aciduria type 1 (GA1, n = 176). Statistical analysis included description and recursive partitioning of diagnostic and therapeutic strategies, and odds ratios (OR) for health outcome parameters. For some analyses, symptomatic patients were divided into those presenting with first symptoms during (i.e. early onset, EO) or after the newborn period (i.e. late onset, LO). Results: Patients identified by newborn screening (NBS) had a significantly lower median age of diagnosis (8 days) compared to the LO group (363 days, p < 0.001], but not compared to the EO group. Of all OAD patients 71 % remained asymptomatic until day 8. Patients with cobalamin-nonresponsive MMA (MMA-Cbl) and GA1 identified by NBS were less likely to have movement disorders than those diagnosed by selective screening (MMA-Cbl: 10 % versus 39 %, p = 0.002; GA1: 26 % versus 73 %, p < 0.001). For other OADs, the clinical benefit of NBS was less clear. Reported age-adjusted intake of natural protein and calories was significantly higher in LO patients than in EO patients reflecting different disease severities. Variable drug combinations, ranging from 12 in MMA-Cbl to two in isovaleric aciduria, were used for maintenance treatment. The effects of specific metabolic treatment strategies on the health outcomes remain unclear because of the strong influences of age at onset (EO versus LO), diagnostic mode (NBS versus selective screening), and the various treatment combinations used. Conclusions: NBS is an effective intervention to reduce time until diagnosis especially for LO patients and to prevent irreversible cerebral damage in GA1 and MMA-Cbl. Huge diversity of therapeutic interventions hampers our understanding of optimal treatment. [ABSTRACT FROM AUTHOR]

Published

2016

13. The phenotypic spectrum of organic acidurias and urea cycle disorders. Part 1: the initial presentation.

Author

Kölker, Stefan, Cazorla, Angeles, Valayannopoulos, Vassili, Lund, Allan, Burlina, Alberto, Sykut-Cegielska, Jolanta, Wijburg, Frits, Teles, Elisa, Zeman, Jiri, Dionisi-Vici, Carlo, Barić, Ivo, Karall, Daniela, Augoustides-Savvopoulou, Persephone, Aksglaede, Lise, Arnoux, Jean-Baptiste, Avram, Paula, Baumgartner, Matthias, Blasco-Alonso, Javier, Chabrol, Brigitte, and Chakrapani, Anupam

Abstract

Background: The clinical presentation of patients with organic acidurias (OAD) and urea cycle disorders (UCD) is variable; symptoms are often non-specific. Aims/methods: To improve the knowledge about OAD and UCD the E-IMD consortium established a web-based patient registry. Results: We registered 795 patients with OAD (n = 452) and UCD (n = 343), with ornithine transcarbamylase (OTC) deficiency (n = 196), glutaric aciduria type 1 (GA1; n = 150) and methylmalonic aciduria (MMA; n = 149) being the most frequent diseases. Overall, 548 patients (69 %) were symptomatic. The majority of them (n = 463) presented with acute metabolic crisis during (n = 220) or after the newborn period (n = 243) frequently demonstrating impaired consciousness, vomiting and/or muscular hypotonia. Neonatal onset of symptoms was most frequent in argininosuccinic synthetase and lyase deficiency and carbamylphosphate 1 synthetase deficiency, unexpectedly low in male OTC deficiency, and least frequently in GA1 and female OTC deficiency. For patients with MMA, propionic aciduria (PA) and OTC deficiency (male and female), hyperammonemia was more severe in metabolic crises during than after the newborn period, whereas metabolic acidosis tended to be more severe in MMA and PA patients with late onset of symptoms. Symptomatic patients without metabolic crises (n = 94) often presented with a movement disorder, mental retardation, epilepsy and psychiatric disorders (the latter in UCD only). Conclusions: The initial presentation varies widely in OAD and UCD patients. This is a challenge for rapid diagnosis and early start of treatment. Patients with a sepsis-like neonatal crisis and those with late-onset of symptoms are both at risk of delayed or missed diagnosis. [ABSTRACT FROM AUTHOR]

Published

2015

14. The phenotypic spectrum of organic acidurias and urea cycle disorders. Part 2: the evolving clinical phenotype.

Author

Kölker, Stefan, Valayannopoulos, Vassili, Burlina, Alberto, Sykut-Cegielska, Jolanta, Wijburg, Frits, Teles, Elisa, Zeman, Jiri, Dionisi-Vici, Carlo, Barić, Ivo, Karall, Daniela, Arnoux, Jean-Baptiste, Avram, Paula, Baumgartner, Matthias, Blasco-Alonso, Javier, Boy, S., Rasmussen, Marlene, Burgard, Peter, Chabrol, Brigitte, Chakrapani, Anupam, and Chapman, Kimberly

Abstract

Background: The disease course and long-term outcome of patients with organic acidurias (OAD) and urea cycle disorders (UCD) are incompletely understood. Aims: To evaluate the complex clinical phenotype of OAD and UCD patients at different ages. Results: Acquired microcephaly and movement disorders were common in OAD and UCD highlighting that the brain is the major organ involved in these diseases. Cardiomyopathy [methylmalonic (MMA) and propionic aciduria (PA)], prolonged QT interval (PA), optic nerve atrophy [MMA, isovaleric aciduria (IVA)], pancytopenia (PA), and macrocephaly [glutaric aciduria type 1 (GA1)] were exclusively found in OAD patients, whereas hepatic involvement was more frequent in UCD patients, in particular in argininosuccinate lyase (ASL) deficiency. Chronic renal failure was often found in MMA, with highest frequency in mut patients. Unexpectedly, chronic renal failure was also observed in adolescent and adult patients with GA1 and ASL deficiency. It had a similar frequency in patients with or without a movement disorder suggesting different pathophysiology. Thirteen patients (classic OAD: 3, UCD: 10) died during the study interval, ten of them during the initial metabolic crisis in the newborn period. Male patients with late-onset ornithine transcarbamylase deficiency were presumably overrepresented in the study population. Conclusions: Neurologic impairment is common in OAD and UCD, whereas the involvement of other organs (heart, liver, kidneys, eyes) follows a disease-specific pattern. The identification of unexpected chronic renal failure in GA1 and ASL deficiency emphasizes the importance of a systematic follow-up in patients with rare diseases. [ABSTRACT FROM AUTHOR]

Published

2015

15. Heterogeneity of follow-up procedures in French and Belgian patients with treated hereditary tyrosinemia type 1: results of a questionnaire and proposed guidelines.

Author

Schiff, Manuel, Broue, Pierre, Chabrol, Brigitte, Laet, Corinne, Habes, Dalila, Mention, Karine, Sarles, Jacques, Spraul, Anne, Valayannopoulos, Vassili, and Ogier de Baulny, Hélène

Abstract

The 1991 introduction of 2-(2-nitro-4-trifluoro-methylbenzyol)-1,3 cyclohexanedione (NTBC) as a treatment for hereditary tyrosinemia type 1 (HT-1), a disorder of tyrosine catabolism, has radically modified the natural history of this disorder. Despite the dramatic improvements in survival, outcomes and quality of life seen with NTBC treatment, HT-1 remains a chronic disorder with several long-term complications, including, a persistent (albeit low) risk of hepatocellular carcinoma and suboptimal neuropsychological outcomes. There remain unsolved key-questions concerning the long-term outcomes of patients with HT-1, which closely depend on the quality of follow-up in these patients. In the absence of published guidelines, we investigated the follow-up methods used for French and Belgian patients with HT-1. A simple questionnaire providing a rapid overview of follow-up procedures was sent to the 19 physicians in charge of HT-1 patients treated with NTBC and low-tyrosine diet in France and Belgium. Several areas of heterogeneity (especially liver imaging, slit lamp examination, neuropsychological evaluation and maximal plasma tyrosine level accepted) were observed. In an attempt to improve long-term management and outcome of patients with HT-1, we proposed follow-up recommendations. [ABSTRACT FROM AUTHOR]

Published

2012

16. Epileptic and nonepileptic features in patients with early onset epileptic encephalopathy and STXBP1 mutations.

Author

Milh, Mathieu, Villeneuve, Nathalie, Chouchane, Mondher, Kaminska, Anna, Laroche, Cécile, Barthez, Marie Anne, Gitiaux, Cyril, Bartoli, Céline, Borges-Correia, Ana, Cacciagli, Pierre, Mignon-Ravix, Cécile, Cuberos, Hélène, Chabrol, Brigitte, and Villard, Laurent

Subjects

EPILEPSY, GENETIC mutation, ELECTROENCEPHALOGRAPHY, SPASMS, MAGNETIC resonance imaging of the brain

Abstract

Summary Purpose: STXBP1 (MUNC18-1) mutations have been associated with various types of epilepsies, mostly beginning early in life. To refine the phenotype associated with STXBP1 aberrations in early onset epileptic syndromes, we studied this gene in a cohort of patients with early onset epileptic encephalopathy. Methods: STXBP1 was screened in a multicenter cohort of 52 patients with early onset epilepsy (first seizure observed before the age of 3 months), no cortical malformation on brain magnetic resonance imaging (MRI), and negative metabolic screening. Three groups of patients could be distinguished in this cohort: (1) Ohtahara syndromes (n = 38); (2) early myoclonic encephalopathies (n = 7); and (3) early onset epileptic encephalopathies that did not match any familiar syndrome (n = 7). None of the patients displayed any cortical malformation on brain MRI and all were screened through multiple video-electroencephalography (EEG) recordings for a time period spanning from birth to their sixth postnatal month. Subsequently, patients had standard EEG or video-EEG recordings. Key Findings: We found five novel STXBP1 mutations in patients for whom video-EEG recordings could be sampled from the beginning of the disease. All patients with a mutation displayed Ohtahara syndrome, since most early seizures could be classified as epileptic spasms and since the silent EEG periods were on average shorter than bursts. However, each patient in addition displayed a particular clinical and EEG feature: In two patients, early seizures were clonic, with very early EEG studies exhibiting relatively low amplitude bursts of activity before progressing into a typical suppression-burst pattern, whereas the three other patients displayed epileptic spasms associated with typical suppression-burst patterns starting from the early recordings. Epilepsy dramatically improved after 6 months and finally disappeared before the end of the first year of life for four patients; the remaining one patient had few seizures until 18 months of age. In parallel, EEG paroxysmal abnormalities disappeared in three patients and decreased in two, giving place to continuous activity with fast rhythms. Each patient displayed frequent nonepileptic movement disorders that could easily be mistaken for epileptic seizures. These movements could be observed as early as the neonatal period and, unlike seizures, persisted during all the follow-up period. Significance: We confirm that STXBP1 is a major gene to screen in cases of Ohtahara syndrome, since it is mutated in >10% of the Ohtahara patients within our cohort. This gene should particularly be tested in the case of a surprising evolution of the patient condition if epileptic seizures and EEG paroxysmal activity disappear and are replaced by fast rhythms after the end of the first postnatal year. [ABSTRACT FROM AUTHOR]

Published

2011

17. Neurologic features and genotype-phenotype correlation in Wolfram syndrome.

Author

Chaussenot, Annabelle, Bannwarth, Sylvie, Rouzier, Cecile, Vialettes, Bernard, Mkadem, Samira Ait El, Chabrol, Brigitte, Cano, Aline, Labauge, Pierre, and Paquis-Flucklinger, Véronique

Subjects

NEUROLOGIC manifestations of general diseases, SYNDROMES, CHILDREN with epilepsy, PHENOTYPES, GENOTYPE-environment interaction, MAGNETIC resonance imaging, COGNITION disorders

Abstract

The article presents a study on the nature and the frequency of the neurologic manifestations of Wolfram syndrome (WS). The study was performed in 59 patients with WS using a detailed clinical study with genotype-phenotype correlation. Results show that 32% of patients with neurologic signs have cognitive impairment, and malformations of cortical development were found on magnetic resonance imaging in epileptic children and diffuse leukoencephalopathy in adult patients.

Published

2011

18. Incidence and natural history of mucopolysaccharidosis type III in France and comparison with United Kingdom and Greece.

Author

Héron, Bénédicte, Mikaeloff, Yann, Froissart, Roseline, Caridade, Guillaume, Maire, Irène, Caillaud, Catherine, Levade, Thierry, Chabrol, Brigitte, Feillet, François, Ogier, Hélène, Valayannopoulos, Vassili, Michelakakis, Helen, Zafeiriou, Dimitrios, Lavery, Lucy, Wraith, Ed, Danos, Olivier, Heard, Jean-Michel, and Tardieu, Marc

Abstract

Sanfilippo syndrome, or mucopolysaccharidosis type III (MPSIII) is a lysosomal storage disease with predominant neurological manifestations in affected children. It is considered heterogeneous with respect to prevalence, clinical presentation, biochemistry (four biochemical forms of the disease referred to as MPSIIIA, B, C, and D are known), and causative mutations. The perspective of therapeutic options emphasizes the need for better knowledge of MPSIII incidence and natural history. We performed parallel retrospective epidemiological studies of patients diagnosed with MSPIII in France (n = 128), UK (n = 126), and Greece (n = 20) from 1990 to 2006. Incidences ranged from 0.68 per 100,000 live-births in France to 1.21 per 100,000 live-births in UK. MPSIIIA, which predominates in France and UK, was absent in Greece, where most patients have MPSIIIB. The study confirmed the large allelic heterogeneity of MPSIIIA and MPSIIIB and detected several yet undescribed mutations. Analysis of clinical manifestations at diagnosis and over a 6-7 years follow-up indicated that almost all patients, whatever the disease subtype, expressed neurological manifestations before the age of 5 years, including language acquisition delay, cognitive delay, and/or abnormal behavior. In contrast to relatively homogeneous early onset manifestations, disease progression showed significant variation depending on subtype and age at diagnosis. Different severities of disease progressions and different allele distribution between France and UK suggested that mutations are not equally deleterious, although genotype-phenotype correlation could not be established. Notwithstanding the rapidity of further clinical deterioration, all MPSIII patients suffer early onset devastating neurological manifestations that deserve early treatment when available. © 2010 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2011

19. Anticipatory postural adjustments in a bimanual load-lifting task in children with developmental coordination disorder.

Author

JOVER, MARIANNE, SCHMITZ, CHRISTINA, CENTELLES, LAURIE, CHABROL, BRIGITTE, and ASSAIANTE, CHRISTINE

Subjects

MOVEMENT disorders, JUVENILE diseases, MOTOR ability, ELECTROMYOGRAPHY, CHILD development, PATIENTS

Abstract

Aim Postural control is a fundamental component of action in which deficits have been shown to contribute to motor difficulties in children with developmental coordination disorder (DCD). The purpose of this study was to examine anticipatory postural adjustments (APAs) in children with DCD in a bimanual load-lifting task. Method Sixteen children with reported motor problems (two females, 14 males; mean age 9y; SD 2y) and 16 typically developing, age-matched children (six females, 10 males; mean age 9y; SD 2y) took part in the study. The task required the children to maintain a stable elbow angle, despite imposed or voluntary unloading of the forearm. APAs were assessed using electromyography and kinematics analysis. Results Although children with DCD could compensate for the consequences of unloading, the results demonstrated that APAs were less efficient in children with DCD than in typically developing children. A positive and significant coefficient of regression between the flexor inhibition latency and the postural stabilization was only found in typically developing children. Interpretation The impaired fine-tuning of the muscle contribution and the poor stabilization performances demonstrate poor predictive modelling in DCD. [ABSTRACT FROM AUTHOR]

Published

2010

20. Spectrum of movement disorders associated with glutaric aciduria type 1: A study of 16 patients.

Author

Gitiaux, Cyril, Roze, Emmanuel, Kinugawa, Kiyoka, Flamand-Rouvière, Constance, Boddaert, Nathalie, Apartis, Emmanuelle, Valayannopoulos, Vassili, Touati, Guy, Motte, Jacques, Devos, David, Mention, Karine, Dobbelaere, Dries, Rodriguez, Diana, Roubertie, Agathe, Chabrol, Brigitte, Feillet, François, Vidailhet, Marie, and Bahi-Buisson, Nadia

Abstract

Glutaric aciduria type 1 (GA1) is an autosomal recessive neurometabolic disorder due to glutaryl CoA dehydrogenase deficiency. Comprehensive descriptions of GA1-associated movement disorders are rare. In order to refine the description of the motor phenotype, we prospectively studied 16 consecutive pediatric and adult GA1 patients, focusing on the movement disorders and their time course. In most patients, generalized dystonia, superimposed on baseline axial hypotonia, remained the predominant feature throughout the disease course. With aging, it tended to evolve from mobile to fixed dystonia and to be associated with akinetic-rigid parkinsonism. Prominent orofacial involvement was a consistent feature in GA1 patients with movement disorders, resulting in speech disorders with features of combined hyperkinetic dysarthria and speech apraxia. The types and outcome of movement disorders in this setting should be taken into consideration during rehabilitation and for patient selection and evaluation in therapeutic trials. © 2008 Movement Disorder Society [ABSTRACT FROM AUTHOR]

Published

2008

21. Brain metabolic impairment in non-cerebral and cerebral forms of x-linked adrenoleukodystrophy by proton MRS: Identification of metabolic patterns by discriminant analysis.

Author

Salvan, Anne-Marie, Confort-Gouny, Sylviane, Chabrol, Brigitte, Cozzone, Patrick J., and Vion-Dury, Jean

Published

1999

22. Non-lethal neonatal neuromuscular variant of glycogenosis type IV with novel GBE1 mutations.

Author

Fernandez, Carla, Halbert, Cécile, De Paula, André Maues, Lacroze, Valerié, Froissart, Roseline, Figarella-Branger, Dominique, Chabrol, Brigitte, and Pellissier, Jean-François

Abstract

We report a recent case of the severe congenital variant of glycogen storage disease type IV with prolonged survival. The patient was found to be a compound heterozygote for two novel mutations, a missense mutation in exon 5 (p.H188P, c.563A>C) and a severe mutation in intron 5 (c.691+2T>C). We propose that the genotype and the quality of medical care may account for the severe but non-lethal phenotype. Muscle Nerve, 2010 [ABSTRACT FROM AUTHOR]

Published

2010

23. Correction to: Impact of age at onset and newborn screening on outcome in organic acidurias.

Author

Heringer, Jana, Valayannopoulos, Vassili, Lund, Allan M., Wijburg, Frits A., Freisinger, Peter, Barić, Ivo, Baumgartner, Matthias R., Burgard, Peter, Burlina, Alberto B., Chapman, Kimberly A., i Saladelafont, Elisenda Cortès, Karall, Daniela, Mühlhausen, Chris, Riches, Victoria, Schiff, Manuel, Sykut-Cegielska, Jolanta, Walter, John H., Zeman, Jiri, Chabrol, Brigitte, and Kölker, Stefan

Abstract

Due to an unfortunate error during the typesetting process, the collaborators were presented incorrectly. [ABSTRACT FROM AUTHOR]

Published

2018

24. Erratum to: The phenotypic spectrum of organic acidurias and urea cycle disorders. Part 1: the initial presentation.

Author

Kölker, Stefan, Cazorla, Angeles, Valayannopoulos, Vassili, Lund, Allan, Burlina, Alberto, Sykut-Cegielska, Jolanta, Wijburg, Frits, Teles, Elisa, Zeman, Jiri, Dionisi-Vici, Carlo, Barić, Ivo, Karall, Daniela, Augoustides-Savvopoulou, Persephone, Aksglaede, Lise, Arnoux, Jean-Baptiste, Avram, Paula, Baumgartner, Matthias, Blasco-Alonso, Javier, Chabrol, Brigitte, and Chakrapani, Anupam

Published

2015

25. Erratum to: The phenotypic spectrum of organic acidurias and urea cycle disorders. Part 2: the evolving clinical phenotype.

Author

Kölker, Stefan, Valayannopoulos, Vassili, Burlina, Alberto, Sykut-Cegielska, Jolanta, Wijburg, Frits, Teles, Elisa, Zeman, Jiri, Dionisi-Vici, Carlo, Barić, Ivo, Karall, Daniela, Arnoux, Jean-Baptiste, Avram, Paula, Baumgartner, Matthias, Blasco-Alonso, Javier, Boy, S., Rasmussen, Marlene, Burgard, Peter, Chabrol, Brigitte, Chakrapani, Anupam, and Chapman, Kimberly

Published

2015

26. Erratum to: ALG6-CDG: a recognizable phenotype with epilepsy, proximal muscle weakness, ataxia and behavioral and limb anomalies.

Author

Morava, Eva, Tiemes, Vera, Thiel, Christian, Seta, Nathalie, Lonlay, Pascale, Klerk, Hans, Mulder, Margot, Rubio-Gozalbo, Estela, Visser, Gepke, Hasselt, Peter, Horovitz, Dafne, Souza, Carolina, Schwartz, Ida, Green, Andrew, Al-Owain, Mohammed, Uziel, Graciella, Sigaudy, Sabine, Chabrol, Brigitte, Spronsen, Franc-Jan, and Steinert, Martin

Published

2016

27. CHCHD10 mutations are not a common cause of SMN1-negative type III/IV spinal motor atrophy.

Author

Morel, Godelieve, Rouzier, Cécile, Chaussenot, Annabelle, Ait‐El‐Mkadem, Samira, Bannwarth, Sylvie, Genin, Emmanuelle C., Augé, Gaëlle, Chabrol, Brigitte, Pouget, Jean, Soriani, Marie Hélène, Sacconi, Sabrina, and Paquis‐Flucklinger, Véronique

Published

2015

28. Aortic dilatation in Cockayne syndrome.

Author

Ovaert C, Cano A, and Chabrol B

Subjects

Cockayne Syndrome complications, Female, Humans, Infant, Aorta pathology, Aortic Valve Insufficiency, Cockayne Syndrome pathology

Abstract

Cockayne syndrome is a rare growth failure and premature aging disorder featuring abnormal ultraviolet sensitivity and impaired transcription-coupled DNA repair. Cardiac involvement has not been described in Cockayne patients except for one recently described case of dilated cardiomyopathy. We describe one patient in whom marked ascending aorta dilatation was observed together with mild aortic regurgitation. Ascending aorta dilatation might be another feature of premature aging in Cockayne syndrome and may require cardiovascular investigation and monitoring., (Copyright 2007 Wiley-Liss, Inc.)

Published

2007