Your search keyword '"M. Koenig"' showing total 25 results

1. Density and Temperature Measurements on Laser Generated Radiative Shocks

Author

Alessandra Benuzzi-Mounaix, Tommaso Vinci, Serge Bouquet, Chantal Stehlé, C. Michaut, M. Kœnig, Dimitri Batani, S. Leygnac, L. Boireau, and Olivier Peyrusse

Subjects

Physics, chemistry.chemical_element, Laser, Temperature measurement, law.invention, Power (physics), Shock (mechanics), Interferometry, Xenon, chemistry, law, Radiative transfer, Atomic physics, Astrophysics::Galaxy Astrophysics, Electronic density

Abstract

This paper presents some recent measurements on radiative shocks generated in a xenon gas cell using high power laser. We show new results on temperature and electronic density, and on radial expansion of the shock at various initial conditions (laser energy and gas pressure). The data obtained are compared with one-dimensional and two-dimensional hydro simulations.

Published

2005

2. Phenotypic variability related to dominant UCHL1 mutations: about three families with optic atrophy and ataxia.

Author

Marelli C, Ramond F, Vignal C, Blanchet C, Frost S, Hao Q, Bocquet B, Nadjar Y, Leboucq N, Taieb G, Benkirane M, Hersent C, Koenig M, and Meunier I

Subjects

Humans, Male, Female, Adult, Middle Aged, Mutation, Optic Atrophy genetics, Ubiquitin Thiolesterase genetics, Pedigree, Phenotype, Ataxia genetics, Ataxia physiopathology

Abstract

Introduction: Ubiquitin C-terminal hydrolase L1 (UCHL1) has been associated with a severe, complex autosomal recessive spastic paraplegia (HSP79) [1] [2] [3] [4]. More recently, UCHL1 loss of function (LoF) variants have been associated to an autosomal dominant disease characterized by late-onset spastic ataxia, neuropathy, and frequent optic atrophy [5]., Methods: Routine clinical care whole-genome (WGS) and exome (ES) sequencing., Results: We present three families with autosomal dominant UCHL1-related disorder. The clinical phenotype mainly associated optic atrophy, mixed cerebellar and sensory ataxia, and possible hearing loss. We delineated two major phenotypes, even within the same family: (1) juvenile severe optic atrophy followed by a later-onset ataxia, or (2) late-onset ataxia with asymptomatic or mild optic atrophy. The families harboured three novel heterozygous variants in UCHL1: two loss of function (p.Lys115AsnfsTer40; c.171_174 + 7del11), and one missense (p.Asp176Asn) involving the catalytic site of the protein and potentially altering the adjacent splice site., Discussion: We confirm the existence of dominantly inherited UCHL1 pathogenic variants. We describe a considerable intrafamilial phenotypic variability, with two main phenotypes. Optic atrophy was consistently present, but with varying degrees of severity. Neither delayed motor or intellectual development, nor dysmorphic features were part of the dominant phenotype in comparison with the autosomal recessive form. The molecular mechanism appears to be haploinsufficiency. UCHL1 monoallelic variants should therefore be considered in any case of early-onset optic atrophy or in late-onset complex ataxic syndrome with asymptomatic optic atrophy., (© 2024. Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2024

3. The inherited cerebellar ataxias: an update.

Author

Coarelli G, Wirth T, Tranchant C, Koenig M, Durr A, and Anheim M

Subjects

Humans, Mutation, Ataxia genetics, Cerebellar Ataxia diagnosis, Cerebellar Ataxia genetics, Cerebellar Ataxia therapy, Friedreich Ataxia diagnosis, Friedreich Ataxia genetics, Friedreich Ataxia therapy, Spinocerebellar Ataxias genetics

Abstract

This narrative review aims at providing an update on the management of inherited cerebellar ataxias (ICAs), describing main clinical entities, genetic analysis strategies and recent therapeutic developments. Initial approach facing a patient with cerebellar ataxia requires family medical history, physical examination, exclusions of acquired causes and genetic analysis, including Next-Generation Sequencing (NGS). To guide diagnosis, several algorithms and a new genetic nomenclature for recessive cerebellar ataxias have been proposed. The challenge of NGS analysis is the identification of causative variant, trio analysis being usually the most appropriate option. Public genomic databases as well as pathogenicity prediction software facilitate the interpretation of NGS results. We also report on key clinical points for the diagnosis of the main ICAs, including Friedreich ataxia, CANVAS, polyglutamine spinocerebellar ataxias, Fragile X-associated tremor/ataxia syndrome. Rarer forms should not be neglected because of diagnostic biomarkers availability, disease-modifying treatments, or associated susceptibility to malignancy. Diagnostic difficulties arise from allelic and phenotypic heterogeneity as well as from the possibility for one gene to be associated with both dominant and recessive inheritance. To complicate the phenotype, cerebellar cognitive affective syndrome can be associated with some subtypes of cerebellar ataxia. Lastly, we describe new therapeutic leads: antisense oligonucleotides approach in polyglutamine SCAs and viral gene therapy in Friedreich ataxia. This review provides support for diagnosis, genetic counseling and therapeutic management of ICAs in clinical practice., (© 2022. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany.)

Published

2023

4. Unravelling the etiology of sporadic late-onset cerebellar ataxia in a cohort of 205 patients: a prospective study.

Author

Bogdan T, Wirth T, Iosif A, Schalk A, Montaut S, Bonnard C, Carre G, Lagha-Boukbiza O, Reschwein C, Albugues E, Demuth S, Landsberger H, Einsiedler M, Parratte T, Nguyen A, Lamy F, Durand H, Fahrer P, Voulleminot P, Bigaut K, Chanson JB, Nicolas G, Chelly J, Cazeneuve C, Koenig M, Bund C, Namer IJ, Kremer S, Calmels N, Tranchant C, and Anheim M

Subjects

Humans, Prospective Studies, Sodium-Phosphate Cotransporter Proteins, Type III, Cerebellar Ataxia epidemiology, Cerebellar Ataxia etiology, Cerebellar Ataxia diagnosis, Spinocerebellar Degenerations complications, Spinocerebellar Ataxias complications, Multiple System Atrophy complications

Abstract

Background: Despite recent progress in the field of genetics, sporadic late-onset (> 40 years) cerebellar ataxia (SLOCA) etiology remains frequently elusive, while the optimal diagnostic workup still needs to be determined. We aimed to comprehensively describe the causes of SLOCA and to discuss the relevance of the investigations., Methods: We included 205 consecutive patients with SLOCA seen in our referral center. Patients were prospectively investigated using exhaustive clinical assessment, biochemical, genetic, electrophysiological, and imaging explorations., Results: We established a diagnosis in 135 (66%) patients and reported 26 different causes for SLOCA, the most frequent being multiple system atrophy cerebellar type (MSA-C) (41%). Fifty-one patients (25%) had various causes of SLOCA including immune-mediated diseases such as multiple sclerosis or anti-GAD antibody-mediated ataxia; and other causes, such as alcoholic cerebellar degeneration, superficial siderosis, or Creutzfeldt-Jakob disease. We also identified 11 genetic causes in 20 patients, including SPG7 (n = 4), RFC1-associated CANVAS (n = 3), SLC20A2 (n = 3), very-late-onset Friedreich's ataxia (n = 2), FXTAS (n = 2), SCA3 (n = 1), SCA17 (n = 1), DRPLA (n = 1), MYORG (n = 1), MELAS (n = 1), and a mitochondriopathy (n = 1) that were less severe than MSA-C (p < 0.001). Remaining patients (34%) had idiopathic late-onset cerebellar ataxia which was less severe than MSA-C (p < 0.01)., Conclusion: Our prospective study provides an exhaustive picture of the etiology of SLOCA and clues regarding yield of investigations and diagnostic workup. Based on our observations, we established a diagnostic algorithm for SLOCA., (© 2022. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany.)

Published

2022

5. Species-specific isotope dilution analysis of monomethylmercury in sediment using GC/ICP-ToF-MS and comparison with ICP-Q-MS and ICP-SF-MS.

Author

Faßbender S, von der Au M, Koenig M, Pelzer J, Piechotta C, Vogl J, and Meermann B

Abstract

A recently introduced inductively coupled plasma-time-of-flight-mass spectrometer (ICP-ToF-MS) shows enhanced sensitivity compared to previous developments and superior isotope ratio precision compared to other ToF and commonly used single-collector ICP-MS instruments. Following this fact, an improvement for isotope dilution ICP-MS using the new instrumentation has been reported. This study aimed at investigating whether this improvement also meets the requirements of species-specific isotope dilution using GC/ICP-MS, where short transient signals are recorded. The results of the analysis of monomethylmercury (MMHg) of a sediment reference material show that isotope ratio precision of ICP-MS instruments equipped with quadrupole, sector-field, and time-of-flight mass analyzers is similar within a broad range of peak signal-to-noise ratio when analyzing one isotopic system. The procedural limit of quantification (LOQ) for MMHg, expressed as mass fraction of Hg being present as MMHg, w(Hg) MMHg , was similar as well for all investigated instruments and ranged between 0.003 and 0.016 μg/kg. Due to the simultaneous detection capability, the ICP-ToF-MS might, however, be more favorable when several isotopic systems are analyzed within one measurement. In a case study, the GC/ICP-ToF-MS coupling was applied for analysis of MMHg in sediments of Finow Canal, a historic German canal heavily polluted with mercury. Mass fractions between 0.180 and 41 μg/kg (w(Hg) MMHg ) for MMHg, and 0.056 and 126 mg/kg (w(Hg) total ) for total mercury were found in sediment samples taken from the canal upstream and downstream of a former chemical plant., (© 2021. The Author(s).)

Published

2021

6. Expanding the clinical spectrum of STIP1 homology and U-box containing protein 1-associated ataxia.

Author

Ravel JM, Benkirane M, Calmels N, Marelli C, Ory-Magne F, Ewenczyk C, Halleb Y, Tison F, Lecocq C, Pische G, Casenave P, Chaussenot A, Frismand S, Tyvaert L, Larrieu L, Pointaux M, Drouot N, Bossenmeyer-Pourié C, Oussalah A, Guéant JL, Leheup B, Bonnet C, Anheim M, Tranchant C, Lambert L, Chelly J, Koenig M, and Renaud M

Subjects

Ataxia, Heat-Shock Proteins, Humans, Mutation genetics, Retrospective Studies, Ubiquitin-Protein Ligases genetics, Cerebellar Ataxia

Abstract

Background: STUB1 has been first associated with autosomal recessive (SCAR16, MIM# 615768) and later with dominant forms of ataxia (SCA48, MIM# 618093). Pathogenic variations in STUB1 are now considered a frequent cause of cerebellar ataxia., Objective: We aimed to improve the clinical, radiological, and molecular delineation of SCAR16 and SCA48., Methods: Retrospective collection of patients with SCAR16 or SCA48 diagnosed in three French genetic centers (Montpellier, Strasbourg and Nancy)., Results: Here, we report four SCAR16 and nine SCA48 patients from two SCAR16 and five SCA48 unrelated French families. All presented with slowly progressive cerebellar ataxia. Additional findings included cognitive decline, dystonia, parkinsonism and swallowing difficulties. The age at onset was highly variable, ranging from 14 to 76 years. Brain MRI showed marked cerebellar atrophy in all patients. Phenotypic findings associated with STUB1 pathogenic variations cover a broad spectrum, ranging from isolated slowly progressive ataxia to severe encephalopathy, and include extrapyramidal features. We described five new pathogenic variations, two previously reported pathogenic variations, and two rare variants of unknown significance in association with STUB1-related disorders. We also report the first pathogenic variation associated with both dominant and recessive forms of inheritance (SCAR16 and SCA48)., Conclusion: Even though differences are observed between the recessive and dominant forms, it appears that a continuum exists between these two entities. While adding new symptoms associated with STUB1 pathogenic variations, we insist on the difficulty of genetic counselling in STUB1-related pathologies. Finally, we underscore the usefulness of DAT-scan as an additional clue for diagnosis.

Published

2021

7. ATP8A2-related disorders as recessive cerebellar ataxia.

Author

Guissart C, Harrison AN, Benkirane M, Oncel I, Arslan EA, Chassevent AK, Baraῆano K, Larrieu L, Iascone M, Tenconi R, Claustres M, Eroglu-Ertugrul N, Calvas P, Topaloglu H, Molday RS, and Koenig M

Subjects

Adult, Child, Child, Preschool, Consanguinity, Female, Genes, Recessive, Humans, Infant, Male, Mutation, Missense, Pedigree, Phenotype, Point Mutation, Adenosine Triphosphatases genetics, Cerebellar Ataxia genetics, Cerebellar Ataxia pathology, Cerebellar Ataxia physiopathology, Phospholipid Transfer Proteins genetics

Abstract

ATP8A2-related disorders are autosomal recessive conditions that associate encephalopathy with or without hypotonia, psychomotor delay, abnormal movements, chorea, tremor, optic atrophy and cerebellar atrophy (CARMQ4). Through a multi-centric collaboration, we identified six point mutations (one splice site and five missense mutations) involving ATP8A2 in six individuals from five families. Two patients from one family with the homozygous p.Gly585Val mutation had a milder presentation without encephalopathy. Expression and functional studies of the missense mutations demonstrated that protein levels of four of the five missense variants were very low and lacked phosphatidylserine-activated ATPase activity. One variant p.Ile215Leu, however, expressed at normal levels and displayed phospholipid-activated ATPase activity similar to the non-mutated protein. We therefore expand for the first time the phenotype related to ATP8A2 mutations to less severe forms characterized by cerebellar ataxia without encephalopathy and suggest that ATP8A2 should be analyzed for all cases of syndromic or non-syndromic recessive or sporadic ataxia.

Published

2020

8. Primitive Dark-Phase Cycle of Photosynthesis at the Origin of Life.

Author

Koenig M

Subjects

Glyceraldehyde chemistry, Phosphorylation, Origin of Life, Phosphates chemistry, Photosynthesis

Abstract

Simple phosphorylation, isomerization, and aldolisation reactions starting from glyceraldehyde have the potential to lead to the synthesis of pre-ribonucleotide polymers through a primitive form of the Calvin cycle (dark phase of photosynthesis) involving the unusual formation of phospho-nonulose phosphate and phospho-deculose phosphate, as key intermediates. These reactions involve activated phosphates which are generated from schreibersite minerals, geochemically available in Hadean times.

Published

2018

9. Deciphering the causes of sporadic late-onset cerebellar ataxias: a prospective study with implications for diagnostic work.

Author

Gebus O, Montaut S, Monga B, Wirth T, Cheraud C, Alves Do Rego C, Zinchenko I, Carré G, Hamdaoui M, Hautecloque G, Nguyen-Them L, Lannes B, Chanson JB, Lagha-Boukbiza O, Fleury MC, Devys D, Nicolas G, Rudolf G, Bereau M, Mallaret M, Renaud M, Acquaviva C, Koenig M, Koob M, Kremer S, Namer IJ, Cazeneuve C, Echaniz-Laguna A, Tranchant C, and Anheim M

Subjects

Adult, Age of Onset, Aged, Brain diagnostic imaging, Calcium Channels genetics, Cerebellar Ataxia genetics, Cerebellar Ataxia pathology, Electromyography, Female, Friedreich Ataxia complications, Humans, Longitudinal Studies, Magnetic Resonance Imaging, Male, Middle Aged, Multiple System Atrophy diagnostic imaging, Mutation genetics, Neural Conduction physiology, Neurologic Examination, Proto-Oncogene Proteins c-sis genetics, Receptor, Platelet-Derived Growth Factor beta genetics, Receptors, G-Protein-Coupled genetics, Receptors, Virus genetics, Retrospective Studies, Severity of Illness Index, Spinocerebellar Ataxias complications, Statistics, Nonparametric, Xenotropic and Polytropic Retrovirus Receptor, Cerebellar Ataxia diagnosis, Cerebellar Ataxia etiology, Multiple System Atrophy complications

Abstract

The management of sporadic late-onset cerebellar ataxias represents a very heterogeneous group of patients and remains a challenge for neurologist in clinical practice. We aimed at describing the different causes of sporadic late-onset cerebellar ataxias that were diagnosed following standardized, exhaustive investigations and the population characteristics according to the aetiologies as well as at evaluating the relevance of these investigations. All patients consecutively referred to our centre due to sporadic, progressive cerebellar ataxia occurring after 40 years of age were included in the prospective, observational study. 80 patients were included over a 2 year period. A diagnosis was established for 52 patients (65%) corresponding to 18 distinct causes, the most frequent being cerebellar variant of multiple system atrophy (n = 29). The second most frequent cause was inherited diseases (including spinocerebellar ataxias, late-onset Friedreich's disease, SLC20A2 mutations, FXTAS, MELAS, and other mitochondrial diseases) (n = 9), followed by immune-mediated or other acquired causes. The group of patient without diagnosis showed a slower worsening of ataxia (p < 0.05) than patients with multiple system atrophy. Patients with later age at onset experienced faster progression of ataxia (p = 0.001) and more frequently parkinsonism (p < 0.05) than patients with earlier onset. Brain MRI, DaT scan, genetic analysis and to some extent muscle biopsy, thoracic-abdominal-pelvic tomodensitometry, and cerebrospinal fluid analysis were the most relevant investigations to explore sporadic late-onset cerebellar ataxia. Sporadic late-onset cerebellar ataxias should be exhaustively investigated to identify the underlying causes that are numerous, including inherited causes, but dominated by multiple system atrophy.

Published

2017

10. Expanding the spectrum of PEX10-related peroxisomal biogenesis disorders: slowly progressive recessive ataxia.

Author

Renaud M, Guissart C, Mallaret M, Ferdinandusse S, Cheillan D, Drouot N, Muller J, Claustres M, Tranchant C, Anheim M, and Koenig M

Subjects

Brain diagnostic imaging, DNA Mutational Analysis, Disability Evaluation, Disease Progression, Female, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Peroxins, Peroxisomal Disorders blood, Peroxisomal Disorders diagnostic imaging, Cerebellar Ataxia genetics, Mutation, Missense genetics, Peroxisomal Disorders genetics, Receptors, Cytoplasmic and Nuclear genetics

Abstract

Peroxisomal biogenesis disorders (PBDs) consist of a heterogeneous group of autosomal recessive diseases, in which peroxisome assembly and proliferation are impaired leading to severe multisystem disease and early death. PBDs include Zellweger spectrum disorders (ZSDs) with a relatively mild clinical phenotype caused by PEX1, (MIM# 602136), PEX2 (MIM# 170993), PEX6 (MIM# 601498), PEX10 (MIM# 602859), PEX12 (MIM# 601758), and PEX16 (MIM# 603360) mutations. Three adult patients are reported belonging to a non-consanguineous French family affected with slowly progressive cerebellar ataxia, axonal neuropathy, and pyramidal signs. Mental retardation and diabetes mellitus were optional. The age at onset was in childhood or in adolescence (3-15 years). Brain MRI showed marked cerebellar atrophy. Biochemical blood analyses suggested a mild peroxisomal defect. With whole exome sequencing, two mutations in PEX10 were found in the three patients: c.827G>T (novel) causing the missense change p.Cys276Phe and c.932G>A causing the missense change p.Arg311Gln. The phenotypic spectrum related to PEX10 mutations includes slowly progressive, syndromic recessive ataxia.

Published

2016

11. Validation of a clinical practice-based algorithm for the diagnosis of autosomal recessive cerebellar ataxias based on NGS identified cases.

Author

Mallaret M, Renaud M, Redin C, Drouot N, Muller J, Severac F, Mandel JL, Hamza W, Benhassine T, Ali-Pacha L, Tazir M, Durr A, Monin ML, Mignot C, Charles P, Van Maldergem L, Chamard L, Thauvin-Robinet C, Laugel V, Burglen L, Calvas P, Fleury MC, Tranchant C, Anheim M, and Koenig M

Subjects

Adolescent, Adult, Age of Onset, Aged, Databases, Genetic, Female, Humans, Male, Middle Aged, Reproducibility of Results, Retrospective Studies, Young Adult, Algorithms, Cerebellar Ataxia diagnosis, Cerebellar Ataxia genetics, Genes, Recessive genetics, High-Throughput Nucleotide Sequencing

Abstract

Establishing a molecular diagnosis of autosomal recessive cerebellar ataxias (ARCA) is challenging due to phenotype and genotype heterogeneity. We report the validation of a previously published clinical practice-based algorithm to diagnose ARCA. Two assessors performed a blind analysis to determine the most probable mutated gene based on comprehensive clinical and paraclinical data, without knowing the molecular diagnosis of 23 patients diagnosed by targeted capture of 57 ataxia genes and high-throughput sequencing coming from a 145 patients series. The correct gene was predicted in 61 and 78 % of the cases by the two assessors, respectively. There was a high inter-rater agreement [K = 0.85 (0.55-0.98) p < 0.001] confirming the algorithm's reproducibility. Phenotyping patients with proper clinical examination, imaging, biochemical investigations and nerve conduction studies remain crucial for the guidance of molecular analysis and to interpret next generation sequencing results. The proposed algorithm should be helpful for diagnosing ARCA in clinical practice.

Published

2016

12. Pitfalls in ataxia with ocular motor apraxia type 1: pseudodominant inheritance and very late onset.

Author

Laurencin C, Anheim M, Larrieu L, Tilikete C, Koenig M, and Thobois S

Subjects

Apraxias genetics, Apraxias physiopathology, Cogan Syndrome physiopathology, Family Health, Humans, Male, Middle Aged, Mutation genetics, Young Adult, Apraxias congenital, Cogan Syndrome genetics, DNA-Binding Proteins genetics, Nuclear Proteins genetics, Psychomotor Performance physiology

Published

2015

13. Erratum to: Combined QCM-D/GE as a tool to characterize stimuli-responsive swelling of and protein adsorption on polymer brushes grafted onto 3D-nanostructures.

Author

Koenig M, Kasputis T, Schmidt D, Rodenhausen KB, Eichhorn KJ, Pannier AK, Schubert M, Stamm M, and Uhlmann P

Published

2015

14. A novel autosomal dominant leukodystrophy with specific MRI pattern.

Author

Corlobé A, Taithe F, Clavelou P, Pierre E, Carra-Dallière C, Ayrignac X, Mouzat K, Lumbroso S, Menjot de Champfleur N, Koenig M, Boespflug-Tanguy O, and Labauge P

Subjects

Adult, Exome, Family Health, Female, Genetic Testing, Glial Fibrillary Acidic Protein genetics, Humans, Lamin Type B genetics, Leukoencephalopathies cerebrospinal fluid, Leukoencephalopathies genetics, Male, Middle Aged, Mutation, Receptor, Notch3, Receptors, Notch genetics, Brain pathology, Leukoencephalopathies diagnosis, Magnetic Resonance Imaging

Abstract

Etiologic diagnosis of adulthood leukodystrophy is challenging in neurologic practice. We describe here the clinico-radiological features of a novel autosomal dominant leukodystrophy in a single family. Clinical and MRI features were recorded in a three generation family. Exome sequencing was performed in two affected relatives and one healthy member. Four total relatives (3 women and 1 man, mean age at onset: 45, range 32-59) were followed: 2 for migraine and 2 for cognitive loss. MRI features were homogeneous in the four affected relatives: extensive and symmetrical white matter hyperintensities on T2-weighted images, with a posterior predominance, involvement of the middle cerebellar peduncles, corpus callosum and the posterior limb of the internal capsules. An extensive metabolic screening was negative. In addition, sequencing of pathogenic genes involved in dominant leukodystrophies (NOTCH3, LMNB1, GFAP, CSF1R) was negative. No mutation has been identified yet with exome sequencing. This report is peculiar because of dominant inheritance, adult onset, highly homogeneous white matter hyperintensities on T2-weighted MR images, predominant in the middle cerebellar peduncles and posterior part of internal capsule and absence of mutation of the genes involved in dominant leukodystrophies.

Published

2015

15. Combined QCM-D/GE as a tool to characterize stimuli-responsive swelling of and protein adsorption on polymer brushes grafted onto 3D-nanostructures.

Author

Koenig M, Kasputis T, Schmidt D, Rodenhausen KB, Eichhorn KJ, Pannier AK, Schubert M, Stamm M, and Uhlmann P

Subjects

Animals, Cattle, Refractometry, Surface Properties, Nanostructures chemistry, Polymers chemistry, Quartz Crystal Microbalance Techniques methods, Serum Albumin, Bovine chemistry, Silicon chemistry

Abstract

A combined setup of quartz crystal microbalance and generalized ellipsometry can be used to comprehensively investigate complex functional coatings comprising stimuli-responsive polymer brushes and 3D nanostructures in a dynamic, noninvasive in situ measurement. While the quartz crystal microbalance detects the overall change in areal mass, for instance, during a swelling or adsorption process, the generalized ellipsometry data can be evaluated in terms of a layered model to distinguish between processes occurring within the intercolumnar space or on top of the anisotropic nanocolumns. Silicon films with anisotropic nanocolumnar morphology were prepared by the glancing angle deposition technique and further functionalized by grafting of poly-(acrylic acid) or poly-(N- isopropylacrylamide) chains. Investigations of the thermoresponsive swelling of the poly-(N-isopropylacrylamide) brush on the Si nanocolumns proved the successful preparation of a stimuli-responsive coating. Furthermore, the potential of these novel coatings in the field of biotechnology was explored by investigation of the adsorption of the model protein bovine serum albumin. Adsorption, retention, and desorption triggered by a change in the pH value is observed using poly-(acrylic acid) functionalized nanostructures, although generalized ellipsometry data revealed that this process occurs only on top of the nanostructures. Poly-(N-isopropylacrylamide) is found to render the nanostructures non-fouling properties.

Published

2014

16. Access-related complications in anterior lumbar surgery in patients over 60 years of age.

Author

Rothenfluh DA, Koenig M, Stokes OM, Behrbalk E, and Boszczyk BM

Subjects

Age Factors, Aged, Aged, 80 and over, Female, Humans, Male, Middle Aged, Postoperative Complications epidemiology, Retroperitoneal Space surgery, Retrospective Studies, Risk Factors, Treatment Outcome, Lumbar Vertebrae surgery, Postoperative Complications etiology, Pseudarthrosis surgery, Scoliosis surgery, Spinal Fusion methods, Spondylosis surgery

Abstract

Purpose: The anterior approach is widely used for access to the lumbar spine in the setting of adult deformity either as a stand-alone procedure or in combined anterior-posterior procedures. Access-related complication rates have so far not been reported in an elderly patient population, in which it has been suggested that anterior lumbar surgery is indicated with caution. Here, the complication rates in patients over 60 years of age are reported., Methods: A retrospective chart review in a consecutive series of 31 patients over 60 years of age and in which a retroperitoneal access to the lumbar spine was performed. All charts including anaesthetic charts were reviewed and the patients' demographics, exact surgical procedure, comorbidities, and potential risk factors, as well as intraoperative and vascular complications noted. Patients who had revision anterior surgery, anterior surgery for tumour resection, trauma or infection were excluded., Results: The average age of patients was 64.9 years, ranging 60-81. Eighteen patients were female and 13 male. The average body mass index was 26.7 ranging 18.5-44.0. The indications for surgery were degenerative scoliosis (12 patients), degenerative spondylosis (7 patients), degenerative spondylolisthesis (5 patients), iatrogenic spondylolisthesis following prior posterior decompression (5 patients), and pseudarthrosis following posterolateral instrumented fusion (2 patients). In 10 patients, a single-level anterior lumbar interbody fusion (ALIF) was carried out (1 L3/4, 5 L4/5, 4 L5/S1) and in 11 patients ALIF was performed on two levels (1 L2-4, 1 L3-5, 9 L4-S1). In three patients, 3 levels from L3 to S1 were approached and in seven patients 4 levels from L2 to S1. Patients with three- and four-level anterior lumbar surgery had higher blood loss than two- and one-level surgery (616 ± 340 vs 439 ± 238, p = 0.036). The overall complication rate was 29% (9/31), which included four vascular injuries and one pulmonary embolism. The vascular complication rate was 13% (4/31) with two arterial and two venous injuries requiring repair. No major blood loss over 2,000 ml occurred., Conclusions: Anterior lumbar surgery in an elderly population does not necessarily have higher overall complication rates than in a younger population. The risk of vascular injury requiring repair was higher, but has not resulted in major blood loss and the procedure therefore can be carried out safely. The overall complication rate and blood loss compare favourably to complication rates in posterior adult deformity procedures.

Published

2014

17. From anti-GAD to ataxia with ocular motor apraxia type 2: through the looking glass.

Author

Mariani LL, Degos B, Honnorat J, Trouillas P, Rabin M, Koenig M, and Anheim M

Subjects

Apraxias congenital, Electromyography, Female, Humans, Longitudinal Studies, Middle Aged, Antibodies blood, Ataxia complications, Ataxia immunology, Cogan Syndrome complications, Glutamate Decarboxylase immunology

Published

2013

18. A modified lead-matrix separation procedure shown for lead isotope analysis in Trojan silver artefacts as an example.

Author

Vogl J, Paz B, Koenig M, and Pritzkow W

Subjects

Archaeology history, Archaeology methods, Bicarbonates chemistry, Chromatography methods, History, Ancient, Isotopes analysis, Isotopes isolation & purification, Lead analysis, Mass Spectrometry methods, Sensitivity and Specificity, Artifacts, Lead isolation & purification, Silver analysis

Abstract

A modified Pb-matrix separation procedure using NH4HCO3 solution as eluent has been developed and validated for determination of Pb isotope amount ratios by thermal ionization mass spectrometry. The procedure is based on chromatographic separation using the Pb·Spec resin and an in-house-prepared NH4HCO3 solution serving as eluent. The advantages of this eluent are low Pb blanks (<40 pg mL(-1)) and the property that NH4HCO3 can be easily removed by use of a heating step (>60 °C). Pb recovery is >95 % for water samples. For archaeological silver samples, however, the Pb recovery is reduced to approximately 50 %, but causes no bias in the determination of Pb isotope amount ratios. The validated procedure was used to determine lead isotope amount ratios in Trojan silver artefacts with expanded uncertainties (k = 2) <0.09 %.

Published

2013

19. Molecular diagnosis of known recessive ataxias by homozygosity mapping with SNP arrays.

Author

H'mida-Ben Brahim D, M'zahem A, Assoum M, Bouhlal Y, Fattori F, Anheim M, Ali-Pacha L, Ferrat F, Chaouch M, Lagier-Tourenne C, Drouot N, Thibaut C, Benhassine T, Sifi Y, Stoppa-Lyonnet D, N'Guyen K, Poujet J, Hamri A, Hentati F, Amouri R, Santorelli FM, Tazir M, and Koenig M

Subjects

Adolescent, Adult, Age of Onset, Ataxia Telangiectasia genetics, Child, Chromosome Mapping, Consanguinity, DNA genetics, DNA Mutational Analysis, Female, Genotype, Heat-Shock Proteins genetics, Homozygote, Humans, Infant, Male, Microsatellite Repeats, Mutation genetics, Oculomotor Nerve Diseases genetics, Polymorphism, Single Nucleotide, Spinocerebellar Degenerations genetics, Young Adult, Cerebellar Ataxia diagnosis, Cerebellar Ataxia genetics

Abstract

The diagnosis of rare inherited diseases is becoming more and more complex as an increasing number of clinical conditions appear to be genetically heterogeneous. Multigenic inheritance also applies to the autosomal recessive progressive cerebellar ataxias (ARCAs), for which 14 genes have been identified and more are expected to be discovered. We used homozygosity mapping as a guide for identification of the defective locus in patients with ARCA born from consanguineous parents. Patients from 97 families were analyzed with GeneChip Mapping 10K or 50K SNP Affymetrix microarrays. We identified six families homozygous for regions containing the autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS) gene, two families homozygous for the ataxia-telangiectasia gene (ATM), two families homozygous for the ataxia with oculomotor apraxia type 1 (AOA1) gene, and one family homozygous for the AOA type 2 (AOA2) gene. Upon direct gene testing, we were able to identify a disease-related mutation in all families but one of the two kindred homozygous at the ATM locus. Although linkage analyses pointed to a single locus on chromosome 11q22.1-q23.1 for this family, clinical features, normal levels of serum alpha-foetoprotein as well as absence of mutations in the ATM gene rather suggest the existence of an additional ARCA-related gene in that interval. While the use of homozygosity mapping was very effective at pointing to the correct gene, it also suggests that the majority of patients harbor mutations either in the genes of the rare forms of ARCA or in genes yet to be identified.

Published

2011

20. Epidemiological, clinical, paraclinical and molecular study of a cohort of 102 patients affected with autosomal recessive progressive cerebellar ataxia from Alsace, Eastern France: implications for clinical management.

Author

Anheim M, Fleury M, Monga B, Laugel V, Chaigne D, Rodier G, Ginglinger E, Boulay C, Courtois S, Drouot N, Fritsch M, Delaunoy JP, Stoppa-Lyonnet D, Tranchant C, and Koenig M

Subjects

Adolescent, Adult, Age of Onset, Brain pathology, Cerebellar Ataxia epidemiology, Cerebellar Ataxia therapy, Cohort Studies, Female, Follow-Up Studies, France, Genes, Recessive, Humans, Magnetic Resonance Imaging methods, Male, Mutation, Myography methods, Prospective Studies, Cerebellar Ataxia genetics

Abstract

While Friedreich's ataxia (FRDA) and ataxia telangiectasia (AT) are known to be the two most frequent forms of autosomal recessive cerebellar ataxia (ARCA), knowledge on the other forms of ARCA has been obtained only recently, and they appear to be rarer. Little is known about the epidemiological features and the relative frequency of the ARCAs and only few data are available about the comparative features of ARCAs. We prospectively studied 102 suspected ARCA cases from Eastern France (including 95 from the Alsace region) between 2002 and 2008. The diagnostic procedure was based on a sequential strategic scheme. We examined the clinical, paraclinical and molecular features of the large cohort of patients and compared features and epidemiology according to molecular diagnosis. A molecular diagnosis could be established for 57 patients; 36 were affected with FRDA, seven with ataxia plus oculomotor apraxia type 2 (AOA2), four with AT, three with ataxia plus oculomotor apraxia type 1 (AOA1), three with Marinesco-Sjögren syndrome, two with autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS), one with ataxia with vitamin E deficiency (AVED) and one with autosomal recessive cerebellar ataxia type 2 (ARCA2). The group of patients with no identified mutation had a significantly lower spinocerebellar degeneration functional score corrected for disease duration (SDFS/DD ratio; p = 0.002) and comprised a significantly higher proportion of cases with onset after 20 years (p < 0.01). Extensor plantar reflexes were rarer and cerebellar atrophy was more frequent in the group of patients with a known non-Friedreich ARCA compared to all other patients (p < 0.0001 and p = 0.0003, respectively). Lower limb areflexia and electroneuromyographic evidences of peripheral neuropathy were more frequent in the Friedreich ataxia group than in the group with a known non-Friedreich ataxia and were more frequent in the later group than in the group with no identified mutation (p = 0.0001 and p = 0.01, respectively). The overall prevalence of ARCA in Alsace is 1/19,000. We can infer the prevalence of FRDA in Alsace to be 1/50,000 and infer that AT is approximately eight times less frequent than FRDA. MSS, AOA2 and ARSACS appear only slightly less frequent than AT. Despite the broad variability of severity, Friedreich ataxia patients are clinically distinct from the other forms of ARCA. Patients with no identified mutation have more often a pure cerebellar degenerative disease or a spastic ataxia phenotype. It appears that ARCA cases can be divided into two major groups of different prognosis, an early-onset group with a highly probable genetic cause and an adult-onset group with better prognosis for which a genetic cause is more difficult to prove but not excluded. ARCAs are rare, early-disabling and genetically heterogeneous diseases dominated by FRDA. Several of the recently identified ARCAs, such as AVED, ARSACS, AOA1, AOA2 and MSS, have a prevalence close to AT and should be searched for extensively irrespective of ethnic origins. The strategic scheme is a useful tool for the diagnosis of ARCAs in clinical practice.

Published

2010

21. SPG11 spastic paraplegia. A new cause of juvenile parkinsonism.

Author

Anheim M, Lagier-Tourenne C, Stevanin G, Fleury M, Durr A, Namer IJ, Denora P, Brice A, Mandel JL, Koenig M, and Tranchant C

Subjects

Adolescent, Adult, DNA Mutational Analysis, Female, Humans, Magnetic Resonance Imaging, Male, Paraplegia pathology, Parkinsonian Disorders complications, Parkinsonian Disorders diagnosis, Polymerase Chain Reaction, Brain pathology, Paraplegia genetics, Parkinsonian Disorders genetics, Parkinsonian Disorders pathology, Proteins genetics

Abstract

Autosomal recessive hereditary spastic paraplegia (AR HSP) with thin corpus callosum (TCC) is a rare neurodegenerative disorder often caused by mutations in the gene encoding for spatacsin at the SPG11 locus on chromosome 15q. The disease is characterized by progressive spastic paraparesis and mental retardation which occur during the first two decades of life and frequently with peripheral neuropathy. Brain magnetic resonance imaging (MRI) reveals typical TCC with periventricular white matter changes. We describe two patients, of Turkish descent, from the same consanguineous family and affected with SPG11 in association with unusual early-onset parkinsonism. Parkinsonism occurred during the very early stages of SPG11 in both patients, being in one the inaugural symptom of the disease presented as a resting tremor with akinesia, rigidity and expressing an initial moderate levodopa-response that progressively weakened. The second patient presented a resting tremor with mild akinesia and no levodopa-response. Both patients were affected with progressive spastic paraparesis which had initially occurred at 15 and 12 years of age, respectively, in association with mild mental retardation and an axonal polyneuropathy. TCC with periventricular white matter changes (PWMC) was evident by MRI and (123)I-ioflupane SPECT was abnormal. Genetic analysis detected for both patients a new c.704&#95;705delAT, p.H235RfsX12 homozygous mutation in SPG11. This report provides evidence that parkinsonism may initiate SPG11-linked HSP TCC and that SPG11 may cause juvenile parkinsonism.

Published

2009

22. Human BAC-mediated rescue of the Friedreich ataxia knockout mutation in transgenic mice.

Author

Sarsero JP, Li L, Holloway TP, Voullaire L, Gazeas S, Fowler KJ, Kirby DM, Thorburn DR, Galle A, Cheema S, Koenig M, Williamson R, and Ioannou PA

Subjects

Animals, Female, Gene Dosage, Genes, Lethal, Genetic Complementation Test, Homozygote, Humans, In Situ Hybridization, Fluorescence, Locomotion, Male, Mice, Phenotype, RNA, Messenger genetics, RNA, Messenger metabolism, Reverse Transcriptase Polymerase Chain Reaction, Transgenes physiology, Chromosomes, Artificial, Bacterial, Friedreich Ataxia genetics, Friedreich Ataxia physiopathology, Mice, Knockout genetics, Mice, Transgenic genetics, Mutation genetics

Abstract

Three independent transgenic mouse lines were generated with the human Friedreich ataxia gene, FRDA, in an 188-kb bacterial artificial chromosome (BAC) genomic sequence. Three copies of the transgene per diploid mouse genome were integrated in a single site in each mouse line. Transgenic mice were mated with mice heterozygous for a knockout mutation of the murine Frda gene, to generate mice homozygous for the Frda knockout mutation and hemizygous or homozygous for the human transgene. Rescue of the embryonic lethality that is associated with homozygosity for the Frda knockout mutation was observed in all three lines. Rescued mice displayed normal behavioral and biochemical parameters. RT-PCR analysis demonstrated that human FRDA mRNA is expressed in all the lines. The relative expression of the human FRDA and mouse Frda genes showed a similar pattern in different tissues in all three lines, indicating position-independent control of expression of the human FRDA transgene. However, large differences in the human:mouse mRNA ratio were observed between different tissues in all three lines. The human transgene is expressed at much higher levels in the brain, liver, and skeletal muscle than the endogenous gene, while expression of the human transgene in blood is only 25-30% of the mouse gene. These studies will facilitate the development of humanized mouse models of Friedreich ataxia through introduction of a GAA trinucleotide expansion or specific known point mutations in the normal human FRDA locus and the study of the regulation of gene expression from the FRDA locus.

Published

2004

23. Rescue of the Friedreich's ataxia knockout mouse by human YAC transgenesis.

Author

Pook MA, Al-Mahdawi S, Carroll CJ, Cossée M, Puccio H, Lawrence L, Clark P, Lowrie MB, Bradley JL, Cooper JM, Koenig M, and Chamberlain S

Subjects

Animals, Disease Models, Animal, Genes, Lethal, Homozygote, Humans, Mice, Phenotype, Phosphotransferases (Alcohol Group Acceptor) genetics, Transgenes genetics, Frataxin, Chromosomes, Artificial, Yeast, Friedreich Ataxia genetics, Friedreich Ataxia physiopathology, Iron-Binding Proteins, Mice, Knockout genetics

Abstract

We have generated and characterised transgenic mice that contain the entire Friedreich's ataxia gene (FRDA) within a human YAC clone of 370 kb. In an effort to overcome the embryonic lethality of homozygous Frda knockout mice and to study the behaviour of human frataxin in a mouse cellular environment, we bred the FRDA YAC transgene onto the null mouse background. Phenotypically normal offspring that express only YAC-derived human frataxin were identified. The human frataxin was expressed in the appropriate tissues at levels comparable to the endogenous mouse frataxin, and it was correctly processed and localised to mitochondria. Biochemical analysis of heart tissue demonstrated preservation of mitochondrial respiratory chain function, together with some increase in citrate synthase and aconitase activities. Thus, we have demonstrated that human frataxin can effectively substitute for endogenous murine frataxin in the null mutant. Our studies are of immediate consequence for the generation of Friedreich's ataxia transgenic mouse models, and further contribute to the accumulating knowledge of human-mouse functional gene replacement systems.

Published

2001

24. Homozygosity mapping of giant axonal neuropathy gene to chromosome 16q24.1.

Author

Ben Hamida C, Cavalier L, Belal S, Sanhaji H, Nadal N, Barhoumi C, M'Rissa N, Marzouki N, Mandel JL, Ben Hamida M, Koenig M, and Hentati F

Subjects

Chromosome Mapping, Family Health, Female, Genetic Linkage, Genetic Predisposition to Disease genetics, Haplotypes, Homozygote, Humans, Male, Microsatellite Repeats, Nervous System Diseases pathology, Pedigree, Axons pathology, Chromosomes, Human, Pair 16 genetics, Nervous System Diseases genetics

Abstract

Giant axonal neuropathy (GAN) is a rare autosomal recessive disorder described as a symmetrical distal neuropathy, with peripheral axons dilated by accumulation of 10 nm neurofilaments (NF) and a severe course of the disease. The observation of kinky or curly hairs is not a constant finding. The GAN1 locus was localized by homozygosity mapping to chromosome 16 q24.1 in a 3 (4) cM interval flanked by the markers D16S3073 and D16S505 (D16S511) in three non-related Tunisian families, showing a genetic homogeneity in these families. Two point lod-score calculation between the linked haplotype and the disease locus was 14.2 at theta(max) = 0. The patients share a slow course of the disease. The differences in the course of the disease between Tunisian and non-Tunisian patients suggest a possible genetic heterogeneity, which is why the present linkage has been referred to as GAN1. The biochemical defect in GAN1 should help to understand the mechanisms involved in NF accumulations as in other neurological diseases (ALS, SMA).

Published

1997

25. Comparison of primary structure of a neuron-specific protein, X11, between human and mouse.

Author

Duclos F and Koenig M

Subjects

Adaptor Proteins, Signal Transducing, Amino Acid Sequence, Animals, Chromosomes, Human, Pair 9, Genes, Humans, Molecular Sequence Data, Sequence Alignment, Sequence Homology, Amino Acid, Species Specificity, Mice genetics, Nerve Tissue Proteins chemistry

Published

1995