Modulation of mammalian spinal motor networks by group I metabotropic glutamate receptors : implications for locomotor control and the motor neuron disease amyotrophic lateral sclerosis

Iwagaki, Noboru

January 2012

The present study examined the role of group I metabotropic glutamate receptors (mGluRs) in mammalian spinal motor networks and investigated the potential role of mGluRs in the fatal neurodegenerative disease amyotrophic lateral sclerosis (ALS). Group I mGluR activation was found to modulate locomotor-related activity recorded from ventral roots of in vitro mouse spinal cord preparations. Activation of group I mGluRs led to an increase in the frequency of locomotor-related bursts and a decrease in their amplitude. The cellular mechanisms underlying group I mGluR-mediated modulation were investigated using whole-cell patch-clamp recordings from spinal neurons. Recordings from motoneurons revealed a wide range of effects, some of which were expected to increase motoneuron excitability, such as membrane depolarisation and hyperpolarisation of action potential thresholds. However, the net modulatory effect of group I mGluR activation was a reduction in motoneuron excitability, likely reflecting a reduction in the density of fast inactivating Na+ currents. The activation of group I mGluRs also reduced excitatory synaptic input to motoneurons, suggesting that modulation of motoneuron properties and synaptic transmission both contribute to group I mGluR-mediated reductions in locomotor motoneuron output. Recordings from spinal interneurons revealed a smaller range of modulatory effects for group I mGluRs. The clearest effect on interneurons, membrane depolarisation, may underlie group I mGluR-mediated increases in the frequency of locomotor activity. Finally, the potential role of group I mGluRs in the pathogenesis of ALS was investigated using a mouse model of the disease. Although no major perturbations in group I mGluR-mediated modulation were demonstrated in ALS affected spinal cords, there appeared to be a difference in the intrinsic excitability of spinal interneurons between wild type and ALS affected animals. Together these data highlight group I mGluRs as important sources of neuromodulation within the spinal cord and potential targets for the treatment of ALS.

616.8

Effekte der präsymptomatischen Applikation der Rho-Kinase-Inhibitoren Fasudil und Y-27632 im SOD1-(G93A)-Mausmodell der Amyotrophen Lateralsklerose / Effects of presymptomatic application of Rho-kinase-Inhibitors Fasudil and Y-27632 in the SOD1(G93A) mouse model of amyotrphic lateral sclerosis

Suhr, Martin Erwin Hermann

21 February 2017

No description available.

610

Rho-kinase

Fasudil

Y-27632

SOD1(G93A) mouse model

presymptomatic

amyotrophic lateral sclerosis

Etude de la jonction neuromusculaire dans la sclérose latérale amyotrophique / A study of neuromuscular junction in amyotrophic lateral sclerosis

Bruneteau, Gaëlle

31 March 2014

La Sclérose Latérale Amyotrophique (SLA) est une affection neurodégénérative touchant les motoneurones, habituellement mortelle en 3 à 5 ans. La cause de la maladie n'est pas connue et le seul traitement actuellement disponible ne permet qu'un allongement modeste de la survie. Des altérations fonctionnelles de la jonction neuromusculaire (JNM) ont été rapportées dans la SLA mais leur origine physiopathologique n'est pas connue. Nous avons étudié les JNM chez 11 patients atteints de SLA, en associant étude morphologique en microscopie confocale et analyse ultrastructurale. L'analyse fonctionnelle réalisée en EMG de surface retrouvait une anomalie de transmission neuromusculaire (décrément > 10%) chez 45% des patients. Des altérations morphologiques des JNM étaient visibles chez tous les patients, y compris au stade précoce de la maladie. Associé aux anomalies en rapport avec le phénomène de dénervation, nous avons observé un aspect anormal de spiculation de la gouttière primaire dans environ un tiers des cas. Une interposition marquée de la cellule de Schwann terminale entre la terminaison nerveuse et la membrane postsynaptique, pouvant altérer la transmission synaptique, était parfois visible. Nous avons objectivé une réinnervation compensatrice significativement plus importante chez les patients présentant une SLA d'évolution lente et montré que certains facteurs moléculaires musculaires comme l'histone déacétylase 4 pourraient jouer un rôle crucial dans la capacité de réinnervation. Ce travail a mis en évidence des altérations morphologiques majeures au niveau des JNM des patients atteints de SLA et a permis d'identifier des cibles thérapeutiques potentielles. / Amyotrophic Lateral Sclerosis (ALS) is a neurodegenerative disorder affecting motor neurons, usually leading to death in 3 to 5 years. The only treatment currently available, riluzole, has a modest effect on survival. Functional alterations of the neuromuscular junction (NMJ) have been reported in ALS, but their pathophysiological significance remains unknown. We studied the morphology of neuromuscular junctions in muscle samples collected from 11 ALS patients, using confocal and electron microscopy. Functional analysis of the NMJs was performed using surface-recording of compound motor action potentials after repetitive nerve stimulation at slow stimulus rate. A significant decrement (>10%), suggesting impairment of the neuromuscular transmission, was present in 45% of the patients. Morphological alterations of the NMJs were present in all ALS patients even at the early-stages. Beside denervation-induced morphological changes, one third of the NMJs showed abnormal spike-like areas of the outer edge of the postsynaptic primary gutter. A marked interposition of the terminal Schwann cell between the nerve terminal and the postsynaptic membrane, which was likely to alter synaptic transmission, was sometimes present. We found a significantly greater compensatory reinnervation in muscle from patients with slowly progressive ALS. Furthermore, we identified that the muscle molecular factor histone deacetylase 4 could play a key role in muscle reinnervation and disease progression in patients with ALS. This work has highlighted the presence of major morphological changes at the NMJs of ALS patients and identified potential new targets for future treatment.

Sclérose latérale amyotrophique

Jonction neuromusculaire

Innervation

HDAC

Cellule de Schwann terminale

Transmission neuromusculaire

Amyotrophic lateral sclerosis

Neuromuscular junction

616

Rôle du muscle squelettique dans la Sclérose Latérale Amyotrophique : apport de modèles transgéniques conditionnels / Role of skeletal muscle in Amyotrophic Lateral Sclerosis

Picchiarelli, Gina

13 September 2018

La sclérose latérale amyotrophique (SLA) est une maladie neurodégénérative dont les premiers symptômes apparaissent généralement vers 60 ans. Elle affecte sélectivement le système moteur et provoque une paralysie progressive amenant au décès du patient par défaillance respiratoire en quelques années. À ce jour, il n’existe aucun traitement curatif, d’où la nécessité de comprendre la physiopathologie de la SLA. Bien que de nombreuses altérations dans le muscle aient été mises en évidence, sa contribution dans la SLA reste à définir. Nous avons montré que FUS est enrichi dans les noyaux sous-synaptiques de façon dépendante de l’innervation. De plus, FUS se lie au promoteur des récepteurs de l’acétylcholine et induit leur transcription de façon dépendante d’ERM. Le mutant FUS, quant à lui, est enrichi dans les noyaux extra-synaptiques et entraîne une toxicité musculaire responsable de l’altération de la jonction neuromusculaire (JNM). Au-delà de la JNM, FUS active MEF2A, de façon dépendante de PRMT1 afin de réguler les fonctions mitochondriales et la différenciation musculaire. La toxicité musculaire de FUS joue donc un rôle clé dans la physiopathologie de la SLA. / Amyotrophic lateral sclerosis is a neurodegenerative whose first symptoms generally appear around age 60. It is characterized by progressive motor neuron degeneration, paralysis and leading to death due to respiratory failure in a few years. Currently, there is no cure so the understanding of ALS physiopathology is necessary. Although many alterations in the muscle have been highlighted, its contribution in ALS remains to be defined. We showed that FUS is enriched in subsynaptic nuclei and this enrichment depended on innervation. Besides, FUS binds directly acetylcholine receptors (AchR) promoter and is required for Ermdependent induction of AChR expression. Conversely, mutant FUS is enriched on extra-synaptic nuclei and induce muscle intrinsic toxicity responsible for neuromuscular junction (NMJ) alteration. Beyond NMJ, FUS is required for muscle mitochondrial function and muscle differentiation through PRMT1-dependent MEF2A activation. Thus, FUS muscular toxicity plays a key role in the ALS physiopathology.

FUS

Jonction neuromusculaire

Muscle

Récepteurs de l’acétylcholine

Amyotrophic lateral sclerosis

FUS

Neuromuscular junction

Muscle

Acetylcholine receptors

572.8

616.83

Rôle du canal chlorure activé par le calcium TMEM16F dans la motricité et implication dans la sclérose latérale amyotrophique / Role of calcium-activated chloride channel TMEM16F in motricity and implication in amyotrophic lateral sclerosis

Soulard, Claire

02 July 2019

Les motoneurones spinaux occupent la place centrale du système moteur. Ils intègrent l’ensemble des informations provenant de système nerveux central et périphérique pour élaborer une commande motrice finale adaptée aux demandes de l’organisme et aux contraintes de l’environnement. En particulier, le seuil de recrutement et la fréquence de décharge des motoneurones sont des paramètres déterminants dans l’élaboration d’un signal approprié à l’intensité de l’effort requis. Il permet de définir l’ordre dans lequel les unités motrices sont recrutées au cours d’une activité physique : des unités motrices de type lent (S) pour le maintien de la posture, aux unités motrices de type rapide pour les efforts d’intensité modérée (FR) et de forte intensité (FF). Cette étude met en évidence l’existence d’un nouvel acteur mis en jeu dans la régulation de l’excitabilité motoneuronale. Il s’agit du canal chlorure activé par le calcium TMEM16F exprimé spécifiquement dans les motoneurones α au niveau des synapses cholinergiques appelées « bouton C ». A l’instar du rôle des boutons C, TMEM16F est nécessaire pour l’exécution d’un effort de forte intensité. En effet, en adéquation avec les enregistrements électrophysiologiques montrant une élévation du seuil de recrutement des motoneurones rapides TMEM16F-/-, la perte de TMEM16F induit des défauts moteurs à l’effort.La sclérose latérale amyotrophique (SLA), est une maladie neurodégénérative conduisant à la mort sélective des motoneurones. Parmi les processus pathologiques décrits, nous savons que l’excitabilité motoneuronale et l’homéostasie calcique constituent des éléments majeurs de la progression de la SLA. Ce sont des facteurs de vulnérabilité qui participent à la dégénérescence séquentielle des motoneurones FF et suivie des motoneurones FR. Étant donné la sensibilité de TMEM16F au calcium et son implication dans la régulation de l’excitabilité motoneuronale, nous avons inhibé l’expression de ce canal dans un modèle murin de SLA SOD1G93A et réalisé une étude longitudinale. Celle-ci met en évidence un effet protecteur de la délétion de TMEM16F qui est dépendant du genre. / Spinal motoneurons have a prominent place in motor system. Motoneurons integrate all inputs from the central and peripheral nervous systems to construct a motor output adapted to the organism's demands and environmental constraints. In particular, recruitment threshold and firing frequency are key motoneuronal parameters in developing an appropriate signal regarding task-dependent demands. During muscle activity, motor units are orderly recruited beginning with slow-type (S) motor units for posture maintenance, followed by fast-type motor units for moderate intensity tasks (FR) and high intensity tasks (FF). Our study highlights a new factor involved in the regulation of motoneuron excitability. This refers to a calcium-activated chloride channel called TMEM16F, specifically expressed in α motoneurons at cholinergic C-bouton synapse. Likewise C-boutons, TMEM16F is required for the procution of high intensity effort. Indeed, in accordance with electrophysiological recordings showing an increase in recruitment threshold of fast TMEM16F-/- motoneurons, TMEM16F loss of function induces motor defects during an effort.Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease leading to the selective death of motoneurons. Among the pathological processes already described, we know that motoneuronal excitability and calcium homeostasis are major features in ALS progression. Those are vulnerability factors which contribute to sequential degeneration starting with FF motoneurons and followed by FR motoneurons. Given the TMEM16F sensitivity to calcium and its involvement in regulating motoneuron excitability, we inhibited its expression in a SOD1G93A mouse model of ALS and conducted a longitudinal study. It highlights a gender-dependent protective effect of TMEM16F loss.

TMEM16F

Motoneurone

Bouton C

Sclérose latérale amyotrophique

Régulation muscarinique

TMEM16F

Motoneuron

C-Bouton

Amyotrophic lateral sclerosis

Muscarinic regulation

Efeito de aldeídos de colesterol na esclerose lateral amiotrófica: estudo em modelo animal e na agregação da SOD1 in vitro / Effect of secosterol aldehydes on Amyotrophic Lateral Sclerosis: study in animal model and SOD1 aggregation in vitro

Dantas, Lucas Souza

29 June 2018

Aldeídos de colesterol (Secosterol A e Secosterol B) têm sido detectados em amostras de cérebro humano e investigados em modelos de doenças neurodegenerativas como possíveis marcadores e intermediários do processo patológico. Estes oxisteróis constituem uma classe de eletrófilos derivados de lipídeos que podem modificar e induzir agregação de proteínas. A esclerose lateral amiotrófica (ELA) é um distúrbio neurodegenerativo associado ao acúmulo de agregados imunorreativos de superóxido dismutase (Cu, Zn-SOD, SOD1). O objetivo deste trabalho foi avaliar a presença de aldeídos de colesterol em ratos modelo ELA e sua capacidade de induzir a formação de agregados de SOD1 in vitro. Aldeídos de colesterol foram analisados no plasma, medula espinhal e córtex motor de ratos ELA. Uma quantidade elevada de Secosterol B foi detectada no córtex motor desses ratos em comparação com animais controle. Adicionalmente, os experimentos in vitro mostraram que Secosterol B e Secosterol A induziram a agregação da SOD1 em uma forma amiloidogênica que se liga à tioflavina T. Esta agregação não foi observada com o colesterol e os seus hidroperóxidos. Usando aldeídos de colesterol marcados com grupo alquinil e um ensaio de click chemistry, foi observado que os agregados de SOD1 estão ligados covalentemente aos aldeídos. A modificação covalente da proteína foi confirmada por análise de MALDI-TOF, que mostrou a adição de até cinco moléculas de aldeídos de colesterol à proteína por base de Schiff. Curiosamente, a análise comparativa com outros eletrófilos derivados de lipídeos (e.g. HHE e HNE) demonstrou que a agregação de SOD1 aumentou proporcionalmente à hidrofobicidade dos aldeídos, observando-se a maioragregação com aldeídos de colesterol. Os sítios de modificação da SOD1 foram caracterizados por nanoLC-MS/MS após digestão da proteína com tripsina, onde foram identificadas lisinas como o principal aminoácido modificado. Em geral, nossos dados mostram que a oxidação do colesterol que leva à produção de aldeídos de colesterol é aumentada no cérebro de ratos ELA e que os aldeídos altamente hidrofóbicos derivados de colesterol podem promover eficientemente modificação e agregação de SOD1. / Secosterol aldehydes (Secosterol B and Secosterol A) have been detected in human brain samples and investigated in models of neurodegenerative diseases as possible markers and intermediates of the pathological process. These oxysterols constitute a class of lipid-derived electrophiles that can modify and induce aggregation of proteins. Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disorder associated with the accumulation of immunoreactive aggregates of superoxide dismutase (Cu, Zn-SOD, SOD1). The objective of this work is to evaluate the presence of secosterol aldehydes in ALS rats and their ability to induce formation of SOD1 aggregates in vitro. Secosterol aldehydes were analyzed in plasma, spinal cord and motor cortex of ALS rats. A higher amount of Secosterol B was detected in the motor cortex of these rats compared to control animals. In addition, in vitro experiments have shown that Secosterol B and Secosterol A induce aggregation of SOD1 into an amyloidogenic form that binds to thioflavin T. This aggregation was not apparent in incubations with cholesterol and its hydroperoxides. Using alkynyl-labeled secosterol aldehydes and a click chemistry assay, it was found that the SOD1 aggregates are covalently linked to the aldehydes. Covalent modification of the protein was confirmed by MALDI-TOF analysis, which showed the addition of up to five molecules of secosterol aldehydes to the protein by Schiff base formation. Interestingly, the comparative analysis with other lipid-derived electrophiles (e.g. HHE and HNE) demonstrated that the aggregation of SOD1 increased according to the hydrophobicity of the aldehydes. Compared to the other electrophiles, a higher SOD1 aggregation was observed with secosterol aldehydes. SOD1 modification sites were characterized by nanoLC-MS/MS afterprotein digestion with trypsin, revealing lysine as the major amino acid modified in these experiments. Collectively, our data show that cholesterol oxidation leads to the production of secosterol aldehydes, which are increased in the brain of ALS rats, and that these highly hydrophobic aldehydes can efficiently promote the modification and aggregation of SOD1.

Aldeídos de colesterol

Amyotrophic Lateral Sclerosis

Doenças neurodegenerativas

Esclerose Lateral Amiotrófica

Neurodegenerative diseases

Secosterol aldehydes

Superoxide dismutase

Superóxido dismutase

Indicação da gastrostomia em pacientes com esclerose lateral amiotrófica: critérios fonoaudiológicos / Indication of gastrostomy for patients with amyotrophic lateral sclerosis: speech-language therapy criteria

Mendes, Amanda Elias

27 May 2015

Introdução: A esclerose lateral amiotrófica (ELA) é uma doença neurodegenerativa progressiva, de etiologia desconhecida, que envolve os neurônios motores do córtex cerebral, do tronco encefálico e da medula espinhal. O comprometimento dos neurônios motores inferiores causa disfagia, distúrbios de fala e outros sintomas, como fraqueza muscular global e sintomas respiratórios. A dificuldade de deglutição ou disfagia pode causar complicações, como pneumonia aspirativa, má nutrição e desidratação, e afeta a qualidade de vida destes pacientes, sendo necessária a indicação de via alternativa de nutrição. Atualmente, esta indicação é dada subjetivamente pelo exame clínico e funcional realizado pela equipe multidisciplinar, de acordo com a deterioração dos parâmetros da função respiratória, do estado nutricional e de comprometimentos na deglutição. Objetivos: objetivo geral: verificar se a redução de pressão de língua pode ser indicadora de necessidade de gastrostomia (GEP) como via alternativa de nutrição em pacientes com diagnóstico de ELA. Objetivos específicos: verificar se há redução significativa nas medidas funcionais e de pressão de lábio, de língua e de bochecha entre o momento da primeira avaliação e da indicação da GEP; avaliar o tempo desde o primeiro sintoma da doença até a indicação da GEP; verificar se o tempo de indicação da GEP foi influenciado por variáveis demográficas, manifestação clínica inicial (espinhal ou bulbar), condições clínicas, medidas funcionais globais e de deglutição, com destaque para pressão de língua, de lábios e de bochechas. Métodos: Foram estudados longitudinalmente 63 pacientes, avaliados do ponto de vista fonoaudiológico com os instrumentos: escala ASHA, escala ALSFRS, avaliação funcional, medida de pressão dos órgãos fonoarticulatórios com o aparelho IOPI, encaminhamento para videoendoscopia da deglutição (VED) e capacidade vital forçada (CVF) no momento da indicação da GEP. Resultados: Os pacientes tinham faixa etária entre 28 e 79 anos (média de 58 anos de idade), com média de 7,04 anos de escolaridade, tempo médio de doença no momento da avaliação inicial de 34,96 meses, 32% manifestação clínica inicial da forma bulbar, 39,5% espinhal membros superiores e 28,5% espinhal membros inferiores, porém, na avaliação fonoaudiológica inicial, todos apresentavam alguma queixa de acometimento bulbar. Cinquenta pacientes foram encaminhados à GEP, 1 foi a óbito e 12 mantiveram dieta via oral exclusiva até o término do estudo. Medidas funcionais e de pressão de língua, lábio e bochecha apresentaram redução significativa no agravamento da ELA (p < 0,001). Dificuldades com líquido espessado: de contenção (p=0,001), de transporte (p=0,005) e de proteção de vias aéreas inferiores (p =0,003), e com a consistência pastosa: contenção na cavidade oral, (p < 0,001) observadas em avaliações clínicas fonoaudiológicas, e a idade (p =0,014) influenciam na indicação de GEP. Conclusão: A medida de pressão de língua pode, portanto, servir como um indicador adicional, objetivo e prático para o exame do prognóstico da funcionalidade da deglutição, e, em particular, da possibilidade ou não de manutenção de vias tradicionais em pacientes com diagnóstico de ELA / Introduction: Amyotrophic lateral sclerosis (ALS) is a progressive neurodegenerative disease of unknown etiology that involves motor neurons from the cerebral cortex, from the brainstem and from the spinal cord. The damage on the lower motor neurons causes dysphagia, speech disorders and other symptoms such as overall muscle weakness and respiratory symptoms. The difficulty in swallowing, or dysphasia, may cause complications such as aspiration pneumonia, malnutrition and dehydration and affects the quality of live of these patients. Thus, it is necessary to indicate and alternative form of nutrition. This indication is currently given subjectively by the clinical and functional evaluation performed by the multidisciplinary team, according to deterioration of respiratory function parameters, nutritional status and swallowing impairments. Objectives: general objective: verify if reduced tongue pressure could indicate the need for gastrostomy (PEG) as an alternative form of nutrition for patients who have been diagnosed with ALS. Specific objectives: verify if there is significant reduction on tongue, lips, and cheeks pressure as well as functional measures between the moment of the first evaluation and the indication of PEG; evaluate the time between the first symptom of the disease and the indication of PEG; verify if the time of the indication of PEG was influenced by demographic variables, initial clinical manifestation (spinal or bulbar forms), clinical conditions, global and swallowing functional measures, highlighting tongue, lips and cheeks pressure. Methods: 63 patients have been longitudinally studied. They have been assessed from the speech-language therapy point of view with the following instruments: ASHA, ALSFRS, functional evaluation, pressure measurement of the phono-articulatory organs with the IOPI, referral to videoendoscopy of swallowing and FVC at the moment of the indication of PEG. Results: The patients, whose ages ranged from 28 to 79 years old (average of 58 years old), had, on average, 7.04 years of education. They had been suffering from the disease for an average of 34.96 months at the time of the first evaluation. 32% showed initial clinical manifestation of the bulbar form, 39.5% upper limbs spinal form and 28.5% lower limbs spinal form. At the initial speech-language therapy assessment, however, all of them showed some sort of complaint regarding bulbar impairment. 50 patients were sent to PEG, 1 died and 12 continued with an oral exclusive diet until the end of this study. Tongue, lips and cheeks as well as functional measures showed significant decrease with the aggravation of ALS (p < 0,001). Difficulties with thickened liquid: with containment (p=0,001), with transport (p=0,005) and with protection of lower airways (p =0,003) and with pasty consistencies: containment in the oral cavity, (p < 0,001) observed in speech-language therapy clinical assessments, as well as age (p =0,014) have influence on the indication of PEG. Conclusion: The measure of the tongue pressure can, therefore, serve as an additional, objective and practical indicator for the evaluation of the prognosis of swallowing functionality, particularly of the possibility or not of maintenance of traditional forms in patients who have been diagnosed with ALS

Amyotrophic lateral sclerosis

Deglutição/fisiopatologia

Deglutition disorders

Esclerose lateral amiotrófica

Gastrostomia

Gastrostomy

Pressão

Pressure, Deglutition/physiopathology

Transtornos de deglutição

Efeito de aldeídos de colesterol na esclerose lateral amiotrófica: estudo em modelo animal e na agregação da SOD1 in vitro / Effect of secosterol aldehydes on Amyotrophic Lateral Sclerosis: study in animal model and SOD1 aggregation in vitro

Lucas Souza Dantas

29 June 2018

Aldeídos de colesterol (Secosterol A e Secosterol B) têm sido detectados em amostras de cérebro humano e investigados em modelos de doenças neurodegenerativas como possíveis marcadores e intermediários do processo patológico. Estes oxisteróis constituem uma classe de eletrófilos derivados de lipídeos que podem modificar e induzir agregação de proteínas. A esclerose lateral amiotrófica (ELA) é um distúrbio neurodegenerativo associado ao acúmulo de agregados imunorreativos de superóxido dismutase (Cu, Zn-SOD, SOD1). O objetivo deste trabalho foi avaliar a presença de aldeídos de colesterol em ratos modelo ELA e sua capacidade de induzir a formação de agregados de SOD1 in vitro. Aldeídos de colesterol foram analisados no plasma, medula espinhal e córtex motor de ratos ELA. Uma quantidade elevada de Secosterol B foi detectada no córtex motor desses ratos em comparação com animais controle. Adicionalmente, os experimentos in vitro mostraram que Secosterol B e Secosterol A induziram a agregação da SOD1 em uma forma amiloidogênica que se liga à tioflavina T. Esta agregação não foi observada com o colesterol e os seus hidroperóxidos. Usando aldeídos de colesterol marcados com grupo alquinil e um ensaio de click chemistry, foi observado que os agregados de SOD1 estão ligados covalentemente aos aldeídos. A modificação covalente da proteína foi confirmada por análise de MALDI-TOF, que mostrou a adição de até cinco moléculas de aldeídos de colesterol à proteína por base de Schiff. Curiosamente, a análise comparativa com outros eletrófilos derivados de lipídeos (e.g. HHE e HNE) demonstrou que a agregação de SOD1 aumentou proporcionalmente à hidrofobicidade dos aldeídos, observando-se a maioragregação com aldeídos de colesterol. Os sítios de modificação da SOD1 foram caracterizados por nanoLC-MS/MS após digestão da proteína com tripsina, onde foram identificadas lisinas como o principal aminoácido modificado. Em geral, nossos dados mostram que a oxidação do colesterol que leva à produção de aldeídos de colesterol é aumentada no cérebro de ratos ELA e que os aldeídos altamente hidrofóbicos derivados de colesterol podem promover eficientemente modificação e agregação de SOD1. / Secosterol aldehydes (Secosterol B and Secosterol A) have been detected in human brain samples and investigated in models of neurodegenerative diseases as possible markers and intermediates of the pathological process. These oxysterols constitute a class of lipid-derived electrophiles that can modify and induce aggregation of proteins. Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disorder associated with the accumulation of immunoreactive aggregates of superoxide dismutase (Cu, Zn-SOD, SOD1). The objective of this work is to evaluate the presence of secosterol aldehydes in ALS rats and their ability to induce formation of SOD1 aggregates in vitro. Secosterol aldehydes were analyzed in plasma, spinal cord and motor cortex of ALS rats. A higher amount of Secosterol B was detected in the motor cortex of these rats compared to control animals. In addition, in vitro experiments have shown that Secosterol B and Secosterol A induce aggregation of SOD1 into an amyloidogenic form that binds to thioflavin T. This aggregation was not apparent in incubations with cholesterol and its hydroperoxides. Using alkynyl-labeled secosterol aldehydes and a click chemistry assay, it was found that the SOD1 aggregates are covalently linked to the aldehydes. Covalent modification of the protein was confirmed by MALDI-TOF analysis, which showed the addition of up to five molecules of secosterol aldehydes to the protein by Schiff base formation. Interestingly, the comparative analysis with other lipid-derived electrophiles (e.g. HHE and HNE) demonstrated that the aggregation of SOD1 increased according to the hydrophobicity of the aldehydes. Compared to the other electrophiles, a higher SOD1 aggregation was observed with secosterol aldehydes. SOD1 modification sites were characterized by nanoLC-MS/MS afterprotein digestion with trypsin, revealing lysine as the major amino acid modified in these experiments. Collectively, our data show that cholesterol oxidation leads to the production of secosterol aldehydes, which are increased in the brain of ALS rats, and that these highly hydrophobic aldehydes can efficiently promote the modification and aggregation of SOD1.

Aldeídos de colesterol

Doenças neurodegenerativas

Esclerose Lateral Amiotrófica

Superóxido dismutase

Amyotrophic Lateral Sclerosis

Neurodegenerative diseases

Secosterol aldehydes

Superoxide dismutase

Avaliação de diferentes compostos contra paralisia e efeitos deletérios em modelo de esclerose lateral amiotrófica em Caenorhabditis elegans / Evaluation of different compounds against paralysis and deleterious effects in a model of amyotrophic lateral sclerosis in Caenorhabditis elegans

Dal Forno, Ana Helena de Castro

17 March 2017

Submitted by Marcos Anselmo (marcos.anselmo@unipampa.edu.br) on 2018-12-03T17:42:10Z No. of bitstreams: 1 ANA HELENA DE CASTRO DAL FORNO.pdf: 1125113 bytes, checksum: bac2174a37c6246d7048e40640b14f02 (MD5) / Approved for entry into archive by Marcos Anselmo (marcos.anselmo@unipampa.edu.br) on 2018-12-03T17:42:22Z (GMT) No. of bitstreams: 1 ANA HELENA DE CASTRO DAL FORNO.pdf: 1125113 bytes, checksum: bac2174a37c6246d7048e40640b14f02 (MD5) / Made available in DSpace on 2018-12-03T17:42:22Z (GMT). No. of bitstreams: 1 ANA HELENA DE CASTRO DAL FORNO.pdf: 1125113 bytes, checksum: bac2174a37c6246d7048e40640b14f02 (MD5) Previous issue date: 2017-03-17 / A esclerose lateral amiotrófica (ELA) é uma doença paralisante e fatal caracterizada por degeneração e morte dos neurônios motores que é geralmente fatal dentro de cinco anos após diagnóstico e sem tratamento eficaz atual. Aproximadamente 10% dos casos de ELA são familiares (ELAf) e cerca de 20% de ELAf estão associados a mutações no gene superóxido dismutase 1 (sod1). Em busca de modelos experimentais alternativos que possam substituir e oferecer novas possibilidades de ensaio de toxicidade xenobiótica, o nematóide Caenorhabditis elegans foi considerado favorável como um valioso organismo bioindicador. Utilizando cepas transgênicas de C. elegans como modelo ELA HA2619, HA2622, HA2425, HA2426 testamos diferentes compostos para avaliar sua eficácia nas alterações resultantes da mutação em modelo da ELA. Foram testados trealose (5 mM) com vitamina E (200 μg/mL) e os compostos orgânicos (1 μM) 4-fenilselanil-7-cloroquinolina (PSQ) e 4-feniltellanil-7-cloroquinolina (PTQ). Nenhum dos tratamentos testados apresentou resultados positivos para o aumento da longevidade ou diminuição na paralisia, o que nos levou a questionar se os tratamentos podem ter desencadeado um aumento dos sintomas e consequentemente uma piora nos vermes. Também observamos que o tratamento com os compostos orgânicos contra o dano oxidativo causado pelo peróxido de hidrogênio (0,6 mM) não foi revertido. Em nossas perspectivas, mais estudos são necessários para encontrar terapias que podem prolongar a longevidade e diminuir ou retardar a paralisia. / Amyotrophic lateral sclerosis (ALS) is a fatal paralytic disorder characterized by degeneration of motorneuron which is generally fatal within five years of diagnosis and with no current effective treatment. Approximately 10% of the ALS cases are familial ALS (fALS) and about 20% of fALS are associated with mutations in the superoxide dismutase 1 gene (sod1). Seeking for alternative experimental models that may substitute and offer new possibilities to assay xenobiotics toxicity, the nematode Caenorhabditis elegans has been found favorable as a valuable bioindicator organism. Using C. elegans transgenic strains as ALS model HA2619, HA2622, HA2425, HA2426 we tested compounds to evaluate the efficacy in treatment of ALS. Trehalose (5mM) with vitamin E (200μg/mL) and the organocompounds (1μM) 4-phenylselanyl-7-chloroquinoline (PSQ) and 4-phenyltellanyl-7-chloroquinoline (PTQ) were tested. None of the treatments tested positive for increased longevity or delayed or decreased paralysis, which led us to wonder if the treatments may have triggered an increase in symptoms and worsening of the worms. We also observed the treatment with the organocompounds against the oxidative damage caused by hydrogen peroxide (0.6mM) was not reversed. In our perspectives further studies are needed to find therapies that may prolong longevity and decrease or delay paralysis.

CNPQ::CIENCIAS BIOLOGICAS

Esclerose lateral amiotrófica

Trealose

Vitamina E

Organocompostos

Caenorhabditis elegans

Amyotrophic lateral sclerosis

Trehalose

Vitamin E

Organocompounds

Caenorhabditis elegans

Correlação clínico-molecular na esclerose lateral amiotrófica fundamentada pelos achados da expressão gênica no nervo extensor curto do hálux / Clinical-molecular correlation in Amyotrophic Lateral Sclerosis based on gene expression findings of the extensor hallucis brevis nerve

Jorge, Frederico Mennucci de Haidar

27 April 2018

A Esclerose Lateral Amiotrófica (ELA) é uma doença neurodegenerativa progressiva e incurável, caracterizada pela perda seletiva dos neurônios motores (NM) superiores e inferiores com uma sobrevida média de 3 anos. As manifestações clínicas dependem da topografia e comprometimento dos NM. De causa desconhecida, descrições apontam para a participação das células gliais (astrócitos, microglia e célula de Schwann) na toxicidade neuronal. A retração precoce do axônio no músculo esquelético sugere a participação da célula de Schwann na morte neuronal retrógrada (dying back). Este estudo descreveu as alterações na expressão gênica no nervo motor extensor curto do hálux ainda funcionante dos pacientes ELA e o ramo motor do nervo acessório de sujeitos-controle (19 ELA, sendo 9 ELA espinhal e 5 ELA bulbar; 5 controles), utilizando-se plataformas expandidas de microarranjos de DNA (microarray) e análises de bioinformática (DAVID e os seus bancos de dados Kyoto Encyclopedia of Genes and Genomes e o Gene Onthology Consorciun Anottation). Os resultados foram validados por PCRq e Redes de Interação de Proteínas foram geradas pelo Cytoscape. Foram encontrados 138 genes diferencialmente expressos entre esses grupos. O ribossomo e a síntese proteica foram apontados como elementos centrais no estudo em eventos relacionados tanto à neurotoxicidade quanto a protetivos. As Redes destacaram o gene EPS8 na ELA (ambas as formas, ELA bulbar e espinhal) em relação aos controles e o gene FAU na ELA bulbar em relação à ELA espinhal. Os genes e as vias apontados neste estudo deverão ser testados como alvos terapêuticos em estudos futuros envolvendo a ELA / Amyotrophic lateral sclerosis (ALS) is an incurable progressive neurodegenerative disease characterized by the selective loss of upper and lower motor neurons (MN), with a median survival of 3 years. Clinical manifestations depend on onset site and involvement of the MN. Although the cause of ALS is unknown, reports point towards the participation of glial cells (astrocytes, microglia and Schwann cells) in the neuronal toxicity. The early retraction of the axonium indicates a participation of the Schwann cells in retrograde neuronal death (dying back). The current study described the abnormalities in the genic expression of the functioning extensor hallucis brevis motor neuron from ALS subjects, and the motor branch of the accessory nerve from control subjects (19 ALS, being 9 spinal and 5 bulbar types; 5 controls), through an expanded platform of DNA microarrays and bioinformatics analyses (DAVID, Kyoto Encyclopedia of Genes and Genomes, and Gene Onthology Consortium Annotation databases). The results were validated by Quantitative PCR (PCRq) and Protein-Protein interaction network generated by Cytoscape. A total of 138 differentially expressed genes were found in these groups. In this study, the ribosome and protein synthesis were pointed as central elements related both to neurotoxicity and protective events. These networks highlighted the EPS8 gene in ALS (in both types, bulbar and spinal) when correlated to controls, and the FAU gene in bulbar ALS in relation to spinal ALS. The genes and pathways identified in this study should be tested as therapeutic targets in future studies approaching ALS

Amyotrophic lateral sclerosis

Biologia molecular

Células de Schwann

Esclerose lateral amiotrófica

Molecular biology

Motor neuron

Neurodegeneração

Neurodegeneration

Neurônio motor

Schwann cells