Your search keyword '"Scekic-Zahirovic, Jelena"' showing total 11 results

1. Degeneration of serotonin neurons triggers spasticity in amyotrophic lateral sclerosis.

Author

El Oussini, Hajer, Scekic‐Zahirovic, Jelena, Vercruysse, Pauline, Marques, Christine, Dirrig‐Grosch, Sylvie, Dieterlé, Stéphane, Picchiarelli, Gina, Sinniger, Jérôme, Rouaux, Caroline, and Dupuis, Luc

Subjects

*AMYOTROPHIC lateral sclerosis, *SEROTONIN, *NEURONS, *SPASTICITY, *ANIMAL models in research

Abstract

Objective: Spasticity occurs in a wide range of neurological diseases, including neurodegenerative diseases, after trauma, and after stroke, and is characterized by increased reflexes leading to muscle hypertonia. Spasticity is a painful symptom and can severely restrict everyday life, but might also participate in maintaining a low level of motor function in severely impaired patients. Constitutive activity of the serotonin receptors 5-HT2B/C is required for the development of spasticity after spinal cord injury and during amyotrophic lateral sclerosis (ALS). We sought here to provide direct evidence for a role of brainstem serotonin neurons in spasticity.Methods: SOD1(G37R) mice expressing a conditional allele of an ALS-linked SOD1 mutation were crossed with Tph2-Cre mice expressing Cre in serotonergic neurons. Measurement of long-lasting reflex using electromyography, behavioral follow-up, and histological techniques was used to characterize spasticity and motor phenotype.Results: Deleting mutant SOD1 expression selectively in brainstem serotonin neurons was sufficient to rescue loss of TPH2 immunoreactivity and largely preserve serotonin innervation of motor neurons in the spinal cord. Furthermore, this abrogated constitutive activity of 5-HT2B/C receptors and abolished spasticity in end-stage mice. Consistent with spasticity mitigating motor symptoms, selective deletion worsened motor function and accelerated the onset of paralysis.Interpretation: Degeneration of serotonin neurons is necessary to trigger spasticity through the 5-HT2B/C receptor. The wide range of drugs targeting the serotonergic system could be useful to treat spasticity in neurological diseases. Ann Neurol 2017;82:444-456. [ABSTRACT FROM AUTHOR]

Published

2017

2. Motor neuron intrinsic and extrinsic mechanisms contribute to the pathogenesis of FUS-associated amyotrophic lateral sclerosis.

Author

Scekic-Zahirovic, Jelena, Oussini, Hajer, Mersmann, Sina, Drenner, Kevin, Wagner, Marina, Sun, Ying, Allmeroth, Kira, Dieterlé, Stéphane, Sinniger, Jérôme, Dirrig-Grosch, Sylvie, René, Frédérique, Dormann, Dorothee, Haass, Christian, Ludolph, Albert, Lagier-Tourenne, Clotilde, Storkebaum, Erik, and Dupuis, Luc

Subjects

*AMYOTROPHIC lateral sclerosis, *MOTOR neurons, *MYELIN

Abstract

Motor neuron-extrinsic mechanisms have been shown to participate in the pathogenesis of ALS-SOD1, one familial form of amyotrophic lateral sclerosis (ALS). It remains unclear whether such mechanisms contribute to other familial forms, such as TDP-43 and FUS-associated ALS. Here, we characterize a single-copy mouse model of ALS- FUS that conditionally expresses a disease-relevant truncating FUS mutant from the endogenous murine Fus gene. We show that these mice, but not mice heterozygous for a Fus null allele, develop similar pathology as ALS- FUS patients and a mild motor neuron phenotype. Most importantly, CRE-mediated rescue of the Fus mutation within motor neurons prevented degeneration of motor neuron cell bodies, but only delayed appearance of motor symptoms. Indeed, we observed downregulation of multiple myelin-related genes, and increased numbers of oligodendrocytes in the spinal cord supporting their contribution to behavioral deficits. In all, we show that mutant FUS triggers toxic events in both motor neurons and neighboring cells to elicit motor neuron disease. [ABSTRACT FROM AUTHOR]

Published

2017

3. Toxic gain of function from mutant FUS protein is crucial to trigger cell autonomous motor neuron loss.

Author

Scekic‐Zahirovic, Jelena, Sendscheid, Oliver, El Oussini, Hajer, Jambeau, Mélanie, Sun, Ying, Mersmann, Sina, Wagner, Marina, Dieterlé, Stéphane, Sinniger, Jérome, Dirrig‐Grosch, Sylvie, Drenner, Kevin, Birling, Marie‐Christine, Qiu, Jinsong, Zhou, Yu, Li, Hairi, Fu, Xiang‐Dong, Rouaux, Caroline, Shelkovnikova, Tatyana, Witting, Anke, and Ludolph, Albert C

Subjects

*MUTANT proteins, *FRONTOTEMPORAL dementia, *AMYOTROPHIC lateral sclerosis, *RNA-binding proteins, *MOTOR neuron diseases, *CYTOPLASM

Abstract

FUS is an RNA-binding protein involved in amyotrophic lateral sclerosis ( ALS) and frontotemporal dementia ( FTD). Cytoplasmic FUS-containing aggregates are often associated with concomitant loss of nuclear FUS. Whether loss of nuclear FUS function, gain of a cytoplasmic function, or a combination of both lead to neurodegeneration remains elusive. To address this question, we generated knockin mice expressing mislocalized cytoplasmic FUS and complete FUS knockout mice. Both mouse models display similar perinatal lethality with respiratory insufficiency, reduced body weight and length, and largely similar alterations in gene expression and mRNA splicing patterns, indicating that mislocalized FUS results in loss of its normal function. However, FUS knockin mice, but not FUS knockout mice, display reduced motor neuron numbers at birth, associated with enhanced motor neuron apoptosis, which can be rescued by cell-specific CRE-mediated expression of wild-type FUS within motor neurons. Together, our findings indicate that cytoplasmic FUS mislocalization not only leads to nuclear loss of function, but also triggers motor neuron death through a toxic gain of function within motor neurons. [ABSTRACT FROM AUTHOR]

Published

2016

4. Serotonin 2B receptor slows disease progression and prevents degeneration of spinal cord mononuclear phagocytes in amyotrophic lateral sclerosis.

Author

El Oussini, Hajer, Scekic-Zahirovic, Jelena, Vercruysse, Pauline, Sinniger, Jérôme, Dirrig-Grosch, Sylvie, Dieterlé, Stéphane, Echaniz-Laguna, Andoni, Larmet, Yves, Thal, Dietmar, Lawson, Roland, Monassier, Laurent, Maroteaux, Luc, Roumier, Anne, Dupuis, Luc, Bayer, Hanna, Müller, Kathrin, Weishaupt, Jochen, Ludolph, Albert, Witting, Anke, and van Rheenen, Wouter

Subjects

*AMYOTROPHIC lateral sclerosis, *SEROTONIN receptors, *SPINAL cord, *MACROPHAGES, *DEGENERATION (Pathology), PREVENTION of disease progression

Abstract

Microglia are the resident mononuclear phagocytes of the central nervous system and have been implicated in the pathogenesis of neurodegenerative diseases such as amyotrophic lateral sclerosis (ALS). During neurodegeneration, microglial activation is accompanied by infiltration of circulating monocytes, leading to production of multiple inflammatory mediators in the spinal cord. Degenerative alterations in mononuclear phagocytes are commonly observed during neurodegenerative diseases, yet little is known concerning the mechanisms leading to their degeneration, or the consequences on disease progression. Here we observed that the serotonin 2B receptor (5-HT), a serotonin receptor expressed in microglia, is upregulated in the spinal cord of three different transgenic mouse models of ALS. In mutant SOD1 mice, this upregulation was restricted to cells positive for CD11b, a marker of mononuclear phagocytes. Ablation of 5-HT receptor in transgenic ALS mice expressing mutant SOD1 resulted in increased degeneration of mononuclear phagocytes, as evidenced by fragmentation of Iba1-positive cellular processes. This was accompanied by decreased expression of key neuroinflammatory genes but also loss of expression of homeostatic microglial genes. Importantly, the dramatic effect of 5-HT receptor ablation on mononuclear phagocytes was associated with acceleration of disease progression. To determine the translational relevance of these results, we studied polymorphisms in the human HTR2B gene, which encodes the 5-HT receptor, in a large cohort of ALS patients. In this cohort, the C allele of SNP rs10199752 in HTR2B was associated with longer survival. Moreover, patients carrying one copy of the C allele of SNP rs10199752 showed increased 5-HT mRNA in spinal cord and displayed less pronounced degeneration of Iba1 positive cells than patients carrying two copies of the more common A allele. Thus, the 5-HT receptor limits degeneration of spinal cord mononuclear phagocytes, most likely microglia, and slows disease progression in ALS. Targeting this receptor might be therapeutically useful. [ABSTRACT FROM AUTHOR]

Published

2016

5. Absence of Subcerebral Projection Neurons Is Beneficial in a Mouse Model of Amyotrophic Lateral Sclerosis.

Author

Burg, Thibaut, Bichara, Charlotte, Scekic‐Zahirovic, Jelena, Fischer, Mathieu, Stuart‐Lopez, Geoffrey, Brunet, Aurore, Lefebvre, François, Cordero‐Erausquin, Matilde, Rouaux, Caroline, Scekic-Zahirovic, Jelena, Stuart-Lopez, Geoffrey, and Cordero-Erausquin, Matilde

Subjects

*AMYOTROPHIC lateral sclerosis, *NEURONS, *DELAYED onset of disease, *HISTOLOGICAL techniques, *PROGNOSIS, *PYRAMIDAL tract, *ANIMAL experimentation, *BIOLOGICAL models, *BRAIN, *COMPARATIVE studies, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *MOTOR neurons, *RESEARCH, *SPINAL cord, *EVALUATION research

Abstract

Objective: Recent studies carried out on amyotrophic lateral sclerosis patients suggest that the disease might initiate in the motor cortex and spread to its targets along the corticofugal tracts. In this study, we aimed to test the corticofugal hypothesis of amyotrophic lateral sclerosis experimentally.Methods: Sod1G86R and Fezf2 knockout mouse lines were crossed to generate a model that expresses a mutant of the murine Sod1 gene ubiquitously, a condition sufficient to induce progressive motor symptoms and premature death, but genetically lacks corticospinal neurons and other subcerebral projection neurons, one of the main populations of corticofugal neurons. Disease onset and survival were recorded, and weight and motor behavior were followed longitudinally. Hyper-reflexia and spasticity were monitored using electromyographic recordings. Neurodegeneration and gliosis were assessed by histological techniques.Results: Absence of subcerebral projection neurons delayed disease onset, reduced weight loss and motor impairment, and increased survival without modifying disease duration. Absence of corticospinal neurons also limited presymptomatic hyper-reflexia, a typical component of the upper motoneuron syndrome.Interpretation: Major corticofugal tracts are crucial to the onset and progression of amyotrophic lateral sclerosis. In the context of the disease, subcerebral projection neurons might carry detrimental signals to their downstream targets. In its entirety, this study provides the first experimental arguments in favor of the corticofugal hypothesis of amyotrophic lateral sclerosis. ANN NEUROL 2020;88:688-702. [ABSTRACT FROM AUTHOR]

Published

2020

6. Evidence that corticofugal propagation of ALS pathology is not mediated by prion-like mechanism.

Author

Scekic-Zahirovic, Jelena, Fischer, Mathieu, Stuart-Lopez, Geoffrey, Burg, Thibaut, Gilet, Johan, Dirrig-Grosch, Sylvie, Marques, Christine, Birling, Marie-Christine, Kessler, Pascal, and Rouaux, Caroline

Subjects

*AMYOTROPHIC lateral sclerosis, *MOTOR neurons, *NEURODEGENERATION, *MOTOR cortex, *SPINAL cord

Abstract

[Display omitted] • Corticospinal neuron degeneration in ALS is cell autonomous. • SOD1G37R excision from corticospinal neurons prevents their degeneration. • Corticospinal neuron rescue does not affect motor death, disease onset or duration. • SOD1G37R excision from corticospinal neurons does not mitigate SOD1 spinal pathology. • Corticofugal spreading of ALS is unlikely to rely on prion-like propagation of misfolded SOD1 protein. Amyotrophic lateral sclerosis (ALS) arises from the combined degeneration of motor neurons (MN) and corticospinal neurons (CSN). Recent clinical and pathological studies suggest that ALS might start in the motor cortex and spread along the corticofugal axonal projections (including the CSN), either via altered cortical excitability and activity or via prion-like propagation of misfolded proteins. Using mouse genetics, we recently provided the first experimental arguments in favour of the corticofugal hypothesis, but the mechanism of propagation remained an open question. To gain insight into this matter, we tested here the possibility that the toxicity of the corticofugal projection neurons (CFuPN) to their targets could be mediated by their cell autonomous-expression of an ALS causing transgene and possible diffusion of toxic misfolded proteins to their spinal targets. We generated a Crym-CreERT2 mouse line to ablate the SOD1G37R transgene selectively in CFuPN. This was sufficient to fully rescue the CSN and to limit spasticity, but had no effect on the burden of misfolded SOD1 protein in the spinal cord, MN survival, disease onset and progression. The data thus indicate that in ALS corticofugal propagation is likely not mediated by prion-like mechanisms, but could possibly rather rely on cortical hyperexcitability. [ABSTRACT FROM AUTHOR]

Published

2021

7. Loss of hypothalamic MCH decreases food intake in amyotrophic lateral sclerosis.

Author

Bolborea, Matei, Vercruysse, Pauline, Daria, Tselmen, Reiners, Johanna C., Alami, Najwa Ouali, Guillot, Simon J., Dieterlé, Stéphane, Sinniger, Jérôme, Scekic-Zahirovic, Jelena, Londo, Amela, Arcay, Hippolyte, Goy, Marc-Antoine, de Tapia, Claudia Nelson, Thal, Dietmar R., Shibuya, Kazumoto, Otani, Ryo, Arai, Kimihito, Kuwabara, Satoshi, Ludolph, Albert C., and Roselli, Francesco

Subjects

*AMYOTROPHIC lateral sclerosis, *FOOD consumption, *WEIGHT loss, *INGESTION, *APPETITE loss, *WEIGHT gain, *SECRETION, *HOMEOSTASIS

Abstract

Amyotrophic lateral sclerosis (ALS) is associated with impaired energy metabolism, including weight loss and decreased appetite which are negatively correlated with survival. Neural mechanisms underlying metabolic impairment in ALS remain unknown. ALS patients and presymptomatic gene carriers have early hypothalamic atrophy. The lateral hypothalamic area (LHA) controls metabolic homeostasis through the secretion of neuropeptides such as orexin/hypocretin and melanin-concentrating hormone (MCH). Here, we show loss of MCH-positive neurons in three mouse models of ALS based on SOD1 or FUS mutations. Supplementation with MCH (1.2 µg/d) through continuous intracerebroventricular delivery led to weight gain in male mutant Sod1G86R mice. MCH supplementation increased food intake, rescued expression of the key appetite-related neuropeptide AgRP (agouti-related protein) and modified respiratory exchange ratio, suggesting increased carbohydrate usage during the inactive phase. Importantly, we document pTDP-43 pathology and neurodegeneration in the LHA of sporadic ALS patients. Neuronal cell loss was associated with pTDP-43-positive inclusions and signs of neurodegeneration in MCH-positive neurons. These results suggest that hypothalamic MCH is lost in ALS and contributes to the metabolic changes, including weight loss and decreased appetite. [ABSTRACT FROM AUTHOR]

Published

2023

8. VAPB/ALS8 MSP Ligands Regulate Striated Muscle Energy Metabolism Critical for Adult Survival in Caenorhabditis elegans.

Author

Han, Sung Min, El Oussini, Hajer, Scekic-Zahirovic, Jelena, Vibbert, Jack, Cottee, Pauline, Prasain, Jeevan K., Bellen, Hugo J., Dupuis, Luc, and Miller, Michael A.

Subjects

*GENETIC mutation, *AMYOTROPHIC lateral sclerosis, *SPINAL muscular atrophy, *MOTOR neuron diseases, *DROSOPHILA

Abstract

Mutations in VAPB/ALS8 are associated with amyotrophic lateral sclerosis (ALS) and spinal muscular atrophy (SMA), two motor neuron diseases that often include alterations in energy metabolism. We have shown that C. elegans and Drosophila neurons secrete a cleavage product of VAPB, the N-terminal major sperm protein domain (vMSP). Secreted vMSPs signal through Roundabout and Lar-like receptors expressed on striated muscle. The muscle signaling pathway localizes mitochondria to myofilaments, alters their fission/fusion balance, and promotes energy production. Here, we show that neuronal loss of the C. elegans VAPB homolog triggers metabolic alterations that appear to compensate for muscle mitochondrial dysfunction. When vMSP levels drop, cytoskeletal or mitochondrial abnormalities in muscle induce elevated DAF-16, the Forkhead Box O (FoxO) homolog, transcription factor activity. DAF-16 promotes muscle triacylglycerol accumulation, increases ATP levels in adults, and extends lifespan, despite reduced muscle mitochondria electron transport chain activity. Finally, Vapb knock-out mice exhibit abnormal muscular triacylglycerol levels and FoxO target gene transcriptional responses to fasting and refeeding. Our data indicate that impaired vMSP signaling to striated muscle alters FoxO activity, which affects energy metabolism. Abnormalities in energy metabolism of ALS patients may thus constitute a compensatory mechanism counterbalancing skeletal muscle mitochondrial dysfunction. [ABSTRACT FROM AUTHOR]

Published

2013

9. Upper and Lower Motor Neuron Degenerations Are Somatotopically Related and Temporally Ordered in the Sod1 Mouse Model of Amyotrophic Lateral Sclerosis.

Author

Marques, Christine, Burg, Thibaut, Scekic-Zahirovic, Jelena, Fischer, Mathieu, Rouaux, Caroline, Ozdinler, P. Hande, and Turner, Bradley

Subjects

*AMYOTROPHIC lateral sclerosis, *MOTOR neurons, *NEURODEGENERATION, *SPINAL cord, *MOTOR cortex

Abstract

Amyotrophic lateral sclerosis (ALS) is a devastating and fatal neurodegenerative disease arising from the combined degeneration of upper motor neurons (UMN) in the motor cortex, and lower motor neurons (LMN) in the brainstem and spinal cord. This dual impairment raises two major questions: (i) are the degenerations of these two neuronal populations somatotopically related? and if yes (ii), where does neurodegeneration start? If studies carried out on ALS patients clearly demonstrated the somatotopic relationship between UMN and LMN degenerations, their temporal relationship remained an unanswered question. In the present study, we took advantage of the well-described Sod1G86R model of ALS to interrogate the somatotopic and temporal relationships between UMN and LMN degenerations in ALS. Using retrograde labelling from the cervical or lumbar spinal cord of Sod1G86R mice and controls to identify UMN, along with electrophysiology and histology to assess LMN degeneration, we applied rigorous sampling, counting, and statistical analyses, and show that UMN and LMN degenerations are somatotopically related and that UMN depletion precedes LMN degeneration. Together, the data indicate that UMN degeneration is a particularly early and thus relevant event in ALS, in accordance with a possible cortical origin of the disease, and emphasize the need to further elucidate the molecular mechanisms behind UMN degeneration, towards new therapeutic avenues. [ABSTRACT FROM AUTHOR]

Published

2021

10. The VAMP-associated protein VAPB is required for cardiac and neuronal pacemaker channel function.

Author

Silbernagel, Nicole, Walecki, Magdalena, Schäfer, Martin K.-H., Kessler, Mirjam, Zobeiri, Mehrnoush, Rinné, Susanne, Kiper, Aytug K., Komadowski, Marlene A., Vowinkel, Kirsty S., Wemhöner, Konstantin, Fortmüller, Lisa, Schewe, Marcus, Dolga, Amalia M., Scekic-Zahirovic, Jelena, Matschke, Lina A., Culmsee, Carsten, Baukrowitz, Thomas, Monassier, Laurent, Ullrich, Nina D., and Dupuis, Luc

Abstract

Hyperpolarization-activated cyclic nucleotide-gated (HCN) channels encode neuronal and cardiac pacemaker currents. The composition of pacemaker channel complexes in different tissues is poorly understood, and the presence of additional HCN modulating subunits was speculated. Here we show that vesicle-associated membrane protein-associated protein B (VAPB), previously associated with a familial form of amyotrophic lateral sclerosis 8, is an essential HCN1 and HCN2 modulator. VAPB significantly increases HCN2 currents and surface expression and has a major influence on the dendritic neuronal distribution of HCN2. Severe cardiac bradycardias in VAPB-deficient zebrafish and VAPB-/- mice highlight that VAPB physiologically serves to increase cardiac pacemaker currents. An altered T-wave morphology observed in the ECGs of VAPB-/- mice supports the recently proposed role of HCN channels for ventricular repolarization. The critical function of VAPB in native pacemaker channel complexes will be relevant for our understanding of cardiac arrhythmias and epilepsies, and provides an unexpected link between these diseases and amyotrophic lateral sclerosis. [ABSTRACT FROM AUTHOR]

Published

2018

11. Alterations in the hypothalamic melanocortin pathway in amyotrophic lateral sclerosis.

Author

Vercruysse, Pauline, Sinniger, Jérôme, Oussini, Hajer El, Scekic-Zahirovic, Jelena, Dieterlé, Stéphane, Dengler, Reinhard, Meyer, Thomas, Zierz, Stephan, Kassubek, Jan, Fischer, Wilhelm, Dreyhaupt, Jens, Grehl, Torsten, Hermann, Andreas, Grosskreutz, Julian, Witting, Anke, Den Bosch, Ludo Van, Spreux-Varoquaux, Odile, El Oussini, Hajer, Van Den Bosch, Ludo, and GERP ALS Study Group

Subjects

*MELANOCORTIN receptors, *AMYOTROPHIC lateral sclerosis, *PIOGLITAZONE, *NEUROSCIENCES, *WEIGHT loss, *ANIMAL experimentation, *CELLULAR signal transduction, *COMPARATIVE studies, *HYPOTHALAMUS, *MICE, *PROTEIN precursors, *SUPEROXIDE dismutase, *THIAZOLIDINEDIONES, *PHARMACODYNAMICS, *RILUZOLE, *THERAPEUTICS

Abstract

Amyotrophic lateral sclerosis, the most common adult-onset motor neuron disease, leads to death within 3 to 5 years after onset. Beyond progressive motor impairment, patients with amyotrophic lateral sclerosis suffer from major defects in energy metabolism, such as weight loss, which are well correlated with survival. Indeed, nutritional intervention targeting weight loss might improve survival of patients. However, the neural mechanisms underlying metabolic impairment in patients with amyotrophic lateral sclerosis remain elusive, in particular due to the lack of longitudinal studies. Here we took advantage of samples collected during the clinical trial of pioglitazone (GERP-ALS), and characterized longitudinally energy metabolism of patients with amyotrophic lateral sclerosis in response to pioglitazone, a drug with well-characterized metabolic effects. As expected, pioglitazone decreased glycaemia, decreased liver enzymes and increased circulating adiponectin in patients with amyotrophic lateral sclerosis, showing its efficacy in the periphery. However, pioglitazone did not increase body weight of patients with amyotrophic lateral sclerosis independently of bulbar involvement. As pioglitazone increases body weight through a direct inhibition of the hypothalamic melanocortin system, we studied hypothalamic neurons producing proopiomelanocortin (POMC) and the endogenous melanocortin inhibitor agouti-related peptide (AGRP), in mice expressing amyotrophic lateral sclerosis-linked mutant SOD1(G86R). We observed lower Pomc but higher Agrp mRNA levels in the hypothalamus of presymptomatic SOD1(G86R) mice. Consistently, numbers of POMC-positive neurons were decreased, whereas AGRP fibre density was elevated in the hypothalamic arcuate nucleus of SOD1(G86R) mice. Consistent with a defect in the hypothalamic melanocortin system, food intake after short term fasting was increased in SOD1(G86R) mice. Importantly, these findings were replicated in two other amyotrophic lateral sclerosis mouse models based on TDP-43 (Tardbp) and FUS mutations. Finally, we demonstrate that the melanocortin defect is primarily caused by serotonin loss in mutant SOD1(G86R) mice. Altogether, the current study combined clinical evidence and experimental studies in rodents to provide a mechanistic explanation for abnormalities in food intake and weight control observed in patients with amyotrophic lateral sclerosis. Importantly, these results also show that amyotrophic lateral sclerosis progression impairs responsiveness to classical drugs leading to weight gain. This has important implications for pharmacological management of weight loss in amyotrophic lateral sclerosis. [ABSTRACT FROM AUTHOR]

Published

2016