Etude IRMf de la plasticité cérébrale des réseaux moteurs et cognitifs dans la Sclérose Latérale Amyotrophique / fMRI study of cerebral plasticity of motor and cognitive networks in Amyotrophic Lateral Sclerosis

Poujois, Aurélia

31 October 2011

Ce travail a porté sur les remaniements corticaux précoces des circuits moteurs et extramoteurs dans la SLA grâce à l’étude des activations IRMf issues de tâches motrices et cognitives. La première partie de nos travaux nous a permis de montrer grâce des tâches simples d’activation motrice en IRMf (1) qu’alors que les patients SLA présentaient un déficit moteur discret, une augmentation des activations corticales est apparue dans les aires sensorimotrices bilatérales du cerveau. (2) Ces modifications précoces de l’activité neuronale étaient corrélées à la latéralisation du déficit moteur du membre ou la prédominance manuelle et surtout, (3) au taux de progression de la maladie à un an et à la survie, suggérant que ce remaniement de l’activité qui correspond probablement à de la plasticité cérébrale a des implications fonctionnelles. Enfin, (4) ce phénomène apparaissait actif puisqu’il s’est poursuivi pendant au moins onze mois. Dans la deuxième partie, nous avons montré lors d’une tâche de fluence verbale silencieuse que (1) les SLA présentaient une suractivation initiale des aires dévolues au processus sémantique avec un renforcement de la connectivité fonctionnelle entre les réseaux (CFR). (2) Au bout de onze mois et alors que l’atteinte des fluences était stable, ce phénomène de compensation s’épuisait avec une diminution conjointe de l’activation des réseaux et de la CFR. La tâche de 2-Back, réalisée alors que les patients ne présentaient pas d’atteinte de la mémoire de travail lors des tests psychométriques, nous a permis de montrer en outre que certains circuits non-moteurs se réorganisaient très précocement chez les patients, alors même qu’ils étaient asymptomatiques / In this work we used motor and cognitive tasks in an fMRI study to explore the early cortical reorganizations of the motor and extra-motor circuits in ALS patients. In a first part, using a simple motor task, we demonstrated (1) that increased cortical BOLD signal changes occurred in specific regions of the brain of ALS patients when their motor deficit was still moderate, and that this early signal changes correlated with (2) the lateralisation of the motor deficit or hand predominance and, more importantly, (3) with the rate of disease progression at one year and survival time, suggesting that modulations of cerebral activity in ALS may have functional implications. Furthermore, (4) this brain plasticity was maintained with time and disease progression during at least eleven months. In a second part, we demonstrated during a silent verbal fluency task (1) that ALS patients presented initially an increased cortical activation of areas devolved to the semantic process with an intensification of the functional network connectivity (FNC). (2) After eleven months and while their performance in tests of verbal fluency was stable, this cerebral compensation ran out with a decrease of the previous cerebral activations and the FNC. A N-back working memory paradigm, realized while the patients did not present any deficit of their working memory, allowed us to show that certain non-motor circuits were reorganized prematurely while patients were still asymptomatic

Sclérose Latérale Amyotrophique

Plasticité cérébrale

IRMf

Connectivité fonctionnelle des réseaux

Réseau sensorimoteur

Réseau par défaut

Fluence verbale

N-Back

Cognition

Analyse en composantes indépendantes

Amyotrophic Lateral Sclerosis

Cerebral plasticity

FMRI

Functional network connectivity

Sensorimotor network

Default-mode network

Verbal fluency

N-Back

Independent Component Analysis

Implication de l'expression et localisation de TDP-43 dans le mécanisme des granules de stress dans la sclérose latérale amyotrophique

Khalfallah, Yousra

08 1900

No description available.

TDP-43

Sclérose Latérale Amyotrophique

Démence Fronto-temporale

Réponse au stress

Granules de Stress

Moelle épinière

Neurones moteurs et corticaux

Astrocytes

G3BP1

ARNm

Vieillissement

Amyotrophic Lateral Sclerosis

Fronto Temporal Dementia

Stress response

Stress granules

Spinal cord

Motor and cortical neurons

Astrocytes

mRNA

Aging

High angular resolution diffusion-weighted magnetic resonance imaging: adaptive smoothing and applications

Metwalli, Nader

07 July 2010

Diffusion-weighted magnetic resonance imaging (MRI) has allowed unprecedented non-invasive mapping of brain neural connectivity in vivo by means of fiber tractography applications. Fiber tractography has emerged as a useful tool for mapping brain white matter connectivity prior to surgery or in an intraoperative setting. The advent of high angular resolution diffusion-weighted imaging (HARDI) techniques in MRI for fiber tractography has allowed mapping of fiber tracts in areas of complex white matter fiber crossings. Raw HARDI images, as a result of elevated diffusion-weighting, suffer from depressed signal-to-noise ratio (SNR) levels. The accuracy of fiber tractography is dependent on the performance of the various methods extracting dominant fiber orientations from the HARDI-measured noisy diffusivity profiles. These methods will be sensitive to and directly affected by the noise. In the first part of the thesis this issue is addressed by applying an objective and adaptive smoothing to the noisy HARDI data via generalized cross-validation (GCV) by means of the smoothing splines on the sphere method for estimating the smooth diffusivity profiles in three dimensional diffusion space. Subsequently, fiber orientation distribution functions (ODFs) that reveal dominant fiber orientations in fiber crossings are then reconstructed from the smoothed diffusivity profiles using the Funk-Radon transform. Previous ODF smoothing techniques have been subjective and non-adaptive to data SNR. The GCV-smoothed ODFs from our method are accurate and are smoothed without external intervention facilitating more precise fiber tractography. Diffusion-weighted MRI studies in amyotrophic lateral sclerosis (ALS) have revealed significant changes in diffusion parameters in ALS patient brains. With the need for early detection of possibly discrete upper motor neuron (UMN) degeneration signs in patients with early ALS, a HARDI study is applied in order to investigate diffusion-sensitive changes reflected in the diffusion tensor imaging (DTI) measures axial and radial diffusivity as well as the more commonly used measures fractional anisotropy (FA) and mean diffusivity (MD). The hypothesis is that there would be added utility in considering axial and radial diffusivities which directly reflect changes in the diffusion tensors in addition to FA and MD to aid in revealing neurodegenerative changes in ALS. In addition, applying adaptive smoothing via GCV to the HARDI data further facilitates the application of fiber tractography by automatically eliminating spurious noisy peaks in reconstructed ODFs that would mislead fiber tracking.

Orientation distribution function (ODF)

Q-ball imaging (QBI)

Smoothing splines on the sphere

Generalized cross-validation (GCV)

Funk-Radon transform (FRT)

Radial diffusivity

Axial diffusivity

Amyotrophic lateral sclerosis (ALS)

Diffusion tensor imaging (DTI)

Magnetic resonance imaging

MRI

Brain mapping

Diagnostic imaging

Diffusion magnetic resonance imaging

Genetics of amyotrophic lateral sclerosis

Belzil, Véronique Valérie

02 1900

La sclérose latérale amyotrophique (SLA) est la maladie des neurones moteurs la plus fréquente, affectant 4-6 individus par 100,000 habitants à l’échelle mondiale. La maladie se caractérise par une faiblesse et une atrophie musculaire suite à la dégénérescence des neurones du cortex moteur, tronc cérébral et moelle épinière. Les personnes atteintes développent les premiers symptômes à l’âge adulte et la maladie progresse sur une période de trois à cinq ans. Il a été répertorié qu’environ 10% des patients ont une histoire familiale de SLA; 90% des gens affectés le sont donc de façon sporadique. La découverte il y a 19 ans de mutations dans le gène zinc/copper superoxide dismutase (SOD1), présentes dans 15-20% des cas familiaux de SLA et environ 2% du total des individus affectés, a été l’événement déclencheur pour la découverte de variations génétiques responsables de la maladie. La recherche sur la génétique de la SLA a connu une progression rapide ces quatre dernières années avec l’identification de mutations dans de nouveaux gènes. Toutefois, même si certains de ces gènes ont été démontrés comme réellement liés à la maladie, la contribution d’autres gènes demeure incertaine puisque les résultats publiés de ceux-ci n’ont pas, à ce jour, été répliqués. Une portion substantielle de cas reste cependant à être génétiquement expliquée, et aucun traitement à ce jour n’a été démontré comme étant efficace pour remédier, atténuer ou prévenir la maladie. Le but du projet de recherche de doctorat était d’identifier de nouveaux gènes mutés dans la SLA, tout en évaluant la contribution de gènes nouvellement identifiés chez une importante cohorte multiethnique de cas familiaux et sporadiques. Les résultats présentés sont organisés en trois sections différentes. Dans un premier temps, la contribution de mutations présentes dans le gène FUS est évaluée chez les patients familiaux, sporadiques et juvéniles de SLA. Précisément, de nouvelles mutations sont rapportées et la proportion de mutations retrouvées chez les cas familiaux et sporadiques de SLA est évaluée. De plus, une nouvelle mutation est rapportée dans un cas juvénile de SLA; cette étude de cas est discutée. Dans un deuxième temps, de nouvelles avenues génétiques sont explorées concernant le gène SOD1. En effet, une nouvelle mutation complexe est rapportée chez une famille française de SLA. De plus, la possibilité qu’une mutation présente dans un autre gène impliqué dans la SLA ait un impact sur l’épissage du gène SOD1 est évaluée. Finalement, la dernière section explique la contribution de nouveaux gènes candidats chez les patients atteints de SLA. Spécifiquement, le rôle des gènes OPTN, SIGMAR1 et SORT1 dans le phénotype de SLA est évalué. Il est souhaité que nos résultats combinés avec les récents développements en génétique et biologie moléculaire permettent une meilleure compréhension du mécanisme pathologique responsable de cette terrible maladie tout en guidant le déploiement de thérapies suite à l’identification des cibles appropriées. / Amyotrophic lateral sclerosis (ALS) is the most common of motor neuron diseases, affecting 4-6 individuals per 100,000 individuals worldwide. ALS is characterized by muscle weakness and atrophy caused by the degeneration of neurons located in the motor cortex, brain stem and spinal cord. This fatal disease generally has an adult onset and progresses over a three to five year period. While 10% of patients affected have a family history of the disease, 90% of cases do not and are considered sporadic. The finding of mutations in the zinc/copper superoxide dismutase gene (SOD1) gene 19 years ago in about 15-20% of familial ALS (FALS) patients and approximately 2% of overall cases developed the interest of identifying rare genetics variants causing the disease. The ALS research field experienced a rapid progression during the last four years as mutations in new genes have been identified. While mutations in some of those new genes have been clearly linked to ALS, the role of others is still questionable and so far has not been positively replicated in other populations. Importantly, a significant portion of cases still need to be genetically explained and, unfortunately, there is still no effective treatment to cure, attenuate or prevent the disease. The aim of this Ph.D research project was to identify new ALS mutated genes while analysing the causative role of other newly identified genes in a large familial and sporadic ALS cohort of different origins. The results presented here are categorized into three different sections. First, the contribution of FUS mutations to familial, sporadic and juvenile ALS is analysed. Specifically, new FUS mutations are reported in ALS cases and the proportions of variants present in the tested familial and sporadic ALS cohorts are assessed. In addition, a new mutation is reported in a juvenile ALS patient, and this interesting case is discussed. Second, new genetic avenues are explored for the SOD1 gene. Precisely, a new and complex SOD1 mutation is reported in a French ALS family. Moreover, the possibility that other ALS mutated genes influence SOD1 splicing events is evaluated. Third, the contribution of new candidate genes is evaluated. Precisely, the contribution of OPTN, SIGMAR1 and SORT1 genes to the ALS phenotype is assessed. Hopefully, our different findings combined with recent developments in genetics and molecular biology will permit a better understanding of the pathological mechanisms involved in the disease and will lead to the identification of the right targets in order to develop appropriate therapeutics for ALS patients.

sclérose latérale amyotrophique

maladie des neurones moteurs

dégénération neuronale

génétique humaine

mutations rares

séquençage de gènes candidats

SOD1

TARDBP

FUS

OPTN

SIGMAR1

SORT1

amyotrophic lateral sclerosis

motor neuron disease

neurodegeneration

human genetics

rare mutations

candidate genes sequencing

Einfluss des Proteinaggregationshemmstoffs anle138b auf Beginn und Verlauf der Amyotrophen Lateralsklerose im transgenen hSOD1-Mausmodell / Influence of the protein aggregation inhibitor anle138b on the beginning and progression of amyotrophic lateral sclerosis in the transgenic hSOD1 mouse model

Thyssen, Stella

24 June 2014

No description available.

610

Amyotrophe Lateralsklerose

Neurodegenerative Erkrankung

Motoneuron

Familiäre ALS

Sporadische ALS

Superoxiddismutase 1

Proteinaggregation

hSOD1-Mausmodell

Anle 138b

Griffkraft

Rotarod

Laufrad

Amyotrophic lateral sclerosis

Neurodegenerative disease

Motor neuron

Familiar ALS

Sporadic ALS

Superoxiddismutase 1

Protein aggregation

hSOD1 mouse model

Anle 138b

Grip Strength

Rotarod

Running Wheel

GOK-MEDIZIN

GOK-MEDIZIN

Oligonucleotide-based therapies for neuromuscular disease

Douglas, Andrew Graham Lim

January 2015

No description available.

616.7

O corpo silencioso e a expressão da vida psíquica no sujeito acometido pela esclerose lateral amiotrófica

Calado, Everton Fabrício

17 February 2010

Made available in DSpace on 2017-06-01T18:08:32Z (GMT). No. of bitstreams: 1 dissertacao_everton_calado.pdf: 1245040 bytes, checksum: f1b176f7ece749c7ff2460c71f70682e (MD5) Previous issue date: 2010-02-17 / Fundação de Amparo a Pesquisa do Estado de Alagoas / This research aims to reflect on the expression of the psychic life of the subject affected by Amyotrophic Lateral Sclerosis (ALS), understood the experience of his "body silenced." By this term to designate that peculiar condition of the subject, with the advancement of the disease, tends to lose as much as the articulation of speech movements, with a severeimpairment in their ability to communicate. We want to understand the psychic expression of this subject from the interaction of caregivers, family members and health professionals in contact with this guy at an advanced stage. The method of clinical-qualitative research (Turato, 2005), whose relevance to human health research is to seek to interpret psychological and sociocultural meanings brought by individuals affected by disease as well as the caregivers, families and professionals. The number of participants was determined by the criterion of saturation (Minayo, 1994), in which the researcher closed the group when a number of interviews already reaches the level of expected information. Free collect testimonies of eight participants, four health professionals with experience in caring for ALS patients: a neurologist and a psychologist, a therapist and a physiotherapist, and four caregivers and / or relatives of people affected by ALS: a daughter of patient, a hired caregiver, wife and widow of a patient. Participants were questioned from both aspects of their interaction with the subject affected by ALS, first, ask how, when living with the subject could perceive, interpret and understand their vicissitudes. Then we question what resources used to establish an intersubjective communication between the health professional, family or carer and the individual affected by ALS. Finally, we consider that the expressionunderstanding of the subject's psychic life with ALS encompasses a gradient ranging from the pragmatic elements relational positions by caregivers whose complement has the effect of the seizure of the subjective contents of the patients / Esta pesquisa tem por objeto refletir sobre a expressão da vida psíquica do sujeito acometido pela Esclerose Lateral Amiotrófica (ELA), compreendida na vivência do seu corpo silenciado . Por esse termo designamos a peculiar condição do sujeito que, com o avanço da doença, tende a perder tanto a articulação da fala quanto dos movimentos, com um grave prejuízo em sua capacidade de se comunicar. Pretendemos compreender a expressão psíquica de tal sujeito a partir da interação dos cuidadores, familiares e profissionais de saúde no convívio com esse sujeito na fase avançada da doença. Utilizamos o método clínicoqualitativo de investigação (Turato, 2005), cuja pertinência à pesquisa humana em saúde está em buscar interpretar significados psicológicos e socioculturais trazidos por sujeitos afetados por doença, bem como dos cuidadores, familiares e profissionais. O número de participantes foi determinado pelo critério de saturação (Minayo, 1994), em que o pesquisador fecha o grupo quando determinado número de entrevistas já alcança o nível de informações esperadas. Coletamos depoimentos livres de oito participantes, sendo quatro profissionais de saúde com experiência no atendimento a casos de ELA: um neurologista, uma psicóloga, uma fonoaudióloga e uma fisioterapeuta, e quatro cuidadores e/ou familiares de pessoas acometidas pela ELA: uma filha de paciente, uma cuidadora contratada, uma esposa e uma viúva de paciente. Os participantes foram questionados a partir de dois aspectos de sua interação com o sujeito acometido pela ELA; em primeiro lugar, perguntamos de que modo, no convívio com o sujeito, conseguiam captar, interpretar e compreender suas vicissitudes. Em seguida, questionamos quais os recursos utilizados para o estabelecimento de uma comunicação intersubjetiva entre este profissional de saúde, familiar ou cuidador e o sujeito acometido pela ELA. Consideramos, finalmente, que a expressão-compreensão de vida psíquica do sujeito com ELA abrange uma gradação que vai desde elementos pragmáticos a posições relacionais por parte cuidadores, cuja complementaridade tem por efeito a apreensão dos conteúdos subjetivos dos pacientes

dissertações

sicologia clínica

psicologia clínica da saúde

cuidadores

dissertations

clinical psychology

amyotrophic side - psychological aspects

neuromuscular diseases - psychological

clinical psychology of health

quality of life - psychological aspects

Caregivers

CNPQ::CIENCIAS HUMANAS::PSICOLOGIA

Optimizing CRISPR/Cas9 for Gene Silencing of SOD1 in Mouse Models of ALS

Kennedy, Zachary C.

09 August 2019

Mutations in the SOD1 gene are the best characterized genetic cause of amyotrophic lateral sclerosis (ALS) and account for ~20% of inherited cases and 1-3% of sporadic cases. The gene-editing tool Cas9 can silence mutant genes that cause disease, but effective delivery of CRISPR-Cas9 to the central nervous system (CNS) remains challenging. Here, I developed strategies using canonical Streptococcus pyogenes Cas9 to silence SOD1. In the first strategy, I demonstrate effectiveness of systemic delivery of guide RNA targeting SOD1 to the CNS in a transgenic mouse model expressing human mutant SOD1 and Cas9. Silencing was observed in both the brain and the spinal cord. In the second strategy, I demonstrate the effectiveness of delivering both guide RNA and Cas9 via two AAVs into the ventricles of the brain of SOD1G93A mice. Silencing was observed in the brain and in motor neurons within the spinal cord. For both strategies, treated mice had prolonged survival when compared to controls. Treated mice also had improvements in grip strength and rotarod function. For ICV treated mice, we detected a benefit of SOD1 silencing using net axonal transport assays, a novel method to detect motor neuron function in mice before onset of motor symptoms. These studies demonstrate that Cas9-mediated genome editing can mediate disease gene silencing in motor neurons and warrants further development for use as a therapeutic intervention for SOD1-linked ALS patients.

CRISPR/Cas9

Cas9

Amyotrophic lateral sclerosis

ALS

Motor Neuron Disease

SOD1

superoxide dismutase

gene therapy

gene editing

AAV

adeno associated vector

adeno-associated vector

AAV9

Biology

Biotechnology

Molecular and Cellular Neuroscience

Musculoskeletal Diseases

Nervous System Diseases

Other Neuroscience and Neurobiology

Therapeutics

Investigating the Effects of Mutant FUS on Stress Response in Amyotrophic Lateral Sclerosis: A Thesis

Kaushansky, Laura J.

14 August 2015

During stress, eukaryotes regulate protein synthesis in part through formation of cytoplasmic, non-membrane-bound complexes called stress granules (SGs). SGs transiently store signaling proteins and stalled translational complexes in response to stress stimuli (e.g. oxidative insult, DNA damage, temperature shifts and ER dysfunction). The functional outcome of SGs is proper translational regulation and signaling, allowing cells to overcome stress. The fatal motor neuron disease Amyotrophic Lateral Sclerosis (ALS) develops in an age-related manner and is marked by progressive neuronal death, with cytoplasmic protein aggregation, excitotoxicity and increased oxidative stress as major hallmarks. Fused in Sarcoma/Translocated in Liposarcoma (FUS) is an RNA-binding protein mutated in ALS with roles in RNA and DNA processing. Most ALS-associated FUS mutations cause FUS to aberrantly localize in the cytoplasm due to a disruption in the nuclear localization sequence. Intriguingly, pathological inclusions in human FUSALS cases contain aggregated FUS as well as several SG-associated proteins. Further, cytoplasmic mutant FUS incorporates into SGs, which increases SG volume and number, delays SG assembly, accelerates SG disassembly, and alters SG dynamics. I posit that mutant FUS association with stress granules is a toxic gain-of-function in ALS that alters the function of SGs by interaction with SG components. Here, I show that mutant FUS incorporates in to SGs via its Cterminal RGG motifs, the methylation of which is not required for this localization. Further, I identify protein interactions specific to full-length mutant FUS under stress conditions that are potentially capable of interacting with FUS in SGs. Finally, I demonstrate a potential change in the protein composition of SGs upon incorporation of mutant FUS. These findings advance the field of ALS and SG biology, thereby providing groundwork for future investigation.

stress granules

Mutant FUS

Amyotrophic Lateral Sclerosis

ALS

Theses, UMMS

Stress, Physiological

Cytoplasmic Granules

Oxidative Stress

RNA-Binding Protein FUS

Cell Biology

Cellular and Molecular Physiology

Molecular and Cellular Neuroscience

Molecular Biology

Nervous System Diseases

Optical Analysis of [Ca²⁺]i and Mitochondrial Signaling Pathways: Implications for the Selective Vulnerability of Motoneurons in Amyotrophic Lateral Sclerosis (ALS) / Optische Analysen von [Ca²⁺]i und mitochondrialen Signalwegen: Untersuchungen zur selektiven Verwundbarkeit von Motoneuronen in der amyotrophen Lateralsklerose (ALS)

Jaiswal, Manoj Kumar

23 January 2008

No description available.

500 Naturwissenschaften allgemein

Mathematics and Computer Science

Amyotrophe Lateralsklerose (ALS)

Superoxid-Dismutase 1 (SOD1)

Motoneuronerkrankungen

Kalzium-Puffer

Mitochondrien

Scheiben des Maushirnstamms

Ca²⁺ imaging

Multiphoton-Lasermikroskopie

Imaging of mitochondrien

Amyotrophic lateral sclerosis (ALS)

Superoxide dismutase 1 (SOD1)

Motoneuron Disease

Calcium buffers

Mitochondria

Brainstem slice

Ca²⁺ imaging

Multiphoton microscopy

Imaging of mitochondria

Biologie

Biology