FONTAINE/STROCHLIC Lab

Neuromuscular Connectivity in health and diseases

Our laboratory aims to understand the cellular and molecular mechanisms underlying neuromuscular synapse assembly and maintenance in physiological and pathological conditions.

The Neuromuscular junction (NMJ) is the contact zone between motor neurons and skeletal muscles. This synapse drives the precise initiation and control of motion. Therefore, much of our behavior and wellness relies on the appropriate functioning of this specialised structure. Neuromuscular transmission deficiency occurs in a large array of rare human diseases including channelopathies, congenital or acquired myasthenia and amyotrophic lateral sclerosis. Most of these pathologies are untreatable and life threatening with devastating economic and societal consequences in terms of loss of quality of life and of the burden of disability. The patients display complex clinical phenotypes mainly characterized by a profound muscle weakness and loss of mobility.

We combine unbiased screens and a large array of functional assays including quantitative morphological imaging, behavioral analysis and electrophysiology using mouse models and/or human-derived specimens to explore the complexity of the trans-synaptic mechanisms controlling neuromuscular connectivity. Our overarching goal is to improve physiopathological knowledge that can be used not only for molecular diagnosis and genetic counselling of families affected with the diseases of interest, but also to design new targets of therapeutic interest.

To achieve this goal, our team is built on an organization that favors tight interactions between practicing neurologists from the Paris Est French reference center for neuromuscular diseases and researchers/research assistants together with a large network of national/international collaborations to share knowledge and expertise.

Team 10

We defined three main aims of research:

1) Characterize the molecular determinants underlying NMJ assembly and maintenance (PI: Laure Strochlic/Julien Messéant).

We have recently identified a new trans-synaptic pathway at the NMJ and developed innovative tools using mouse genetics to dissect its molecular characteristics.

2) Understand how disruption of nerve/muscle communication leads to neuromuscular diseases such as myasthenia and amyotrophic lateral sclerosis (PI: Stéphanie Godard-Bauché/Gaelle Bruneteau).

Thanks to our clinical expertise and our national networks, we analyze the physiopathological mechanisms underlying the studied diseases in patients.

3) Modulate trans-synaptic function to restore appropriate synaptic connectivity in a pathological context as a basis for therapeutic interventions (PI: Bertrand Fontaine/Laure Strochlic).

We develop innovative pharmacological or genetic strategies that promote trans-synaptic communication and nerve/muscle attachment to mitigate NMJ disease symptoms to ultimately prevent or compensate the progression of the loss of motor function in neuromuscular diseases.

Key words: Neuromuscular Junction, Neuromuscular disorders, disease modeling mouse models, human derived specimens, quantitative imaging, therapeutic strategies.

Main collaborations:

  • Rozen Le Panse and Sonia Berrih-Aknin (France)
  • Arnaud Ferry (France)
  • Cécile Martinat (France)
  • Eric Krejci (France)
  • Frédérique Charbonnier (France)
  • Nathalie Sans and Mireille Montcouquiol (France)
  • Laurent Schaeffer, NeuroMyoGene Institute, (France)
  • Hanns Lochmüller, The Children’s Hospital of Eastern Ontario (Canada)
  • Markus Ruëgg, Biozentrum (Switzerland)
  • Anna Punga, Uppsala University, (Sweden)

 

 

 

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106 documents

  • Piera Smeriglio. Deregulation of TET/5hmC axis in motor neuron diseases. Epigenetic in muscle disease workshop, Jun 2022, PARIS, France. ⟨hal-04002798⟩
  • Charles Frison-Roche, Steve Cottin, Jeanne Lainé, Ludovic Arandel, Marius Halliez, et al.. MBNL loss of function in the motor unit alters neuromuscular communication. International Myotonic Dystrophy Consortium Meeting IDMC-13, International Myotonic Dystrophy Consortium, May 2022, Osaka, Japan. ⟨hal-04005805⟩
  • Myriam Boëx, Steve Cottin, Marius Halliez, Stéphanie Bauché, Céline Buon, et al.. The cell polarity protein Vangl2 in the muscle shapes the neuromuscular synapse by binding to and regulating the tyrosine kinase MuSK. Science Signaling, 2022, 15 (734), pp.eabg4982. ⟨10.1126/scisignal.abg4982⟩. ⟨inserm-03768653⟩
  • Massiré Traoré, Chiara Noviello, Gentil Christel, Julien Messéant, Ericky Caldas, et al.. Therapeutic approach based on GDF5 to counteract age-related muscle wasting. Muscle formation, maintenance, regeneration and pathology-EMBO workshop, Apr 2022, Gouvieux (FR), France. ⟨hal-04002159⟩
  • Gaëlle Bruneteau. Réseau ACT4ALS-MND - Actualités et perspectives - Essais thérapeutiques. Journées nationales annuelles de la filière de santé maladies rares FILSLAN, 2022, Montpellier, France. ⟨hal-04015822⟩
  • Strochlic Laure. Wnt signaling in Myasthenia. Guarda meeting on the neuromuscular junction, 2022, Guarda, Switzerland. ⟨hal-04002946⟩
  • Halliez Marius, Cottin Steve, You Axel, Lemaitre Mégane, Ezan Jérome, et al.. MUSK CYSTEIN RICH DOMAIN IN AUTOIMMUNE MYASTHENIC SYNDROME. 14th MGFA International Conference On Myasthenia And Related Disorders, 2022, Miami (Florida), United States. ⟨hal-04002779⟩
  • Konstantinos Savvatis, Christoffer Rasmus Vissing, Lori Klouvi, Anca Rezeda Florian, Mehjabin Rahman, et al.. Cardiac Outcomes in Adults With Mitochondrial Diseases. Journal of the American College of Cardiology, 2022, 80 (15), pp.1421-1430. ⟨10.1016/j.jacc.2022.08.716⟩. ⟨hal-03837169⟩
  • Halliez Marius, Cottin Steve, You Axel, Lemaitre Mégane, Ezan Jérome, et al.. MUSK CYSTEIN RICH DOMAIN IN AUTOIMMUNE MYASTHENIC SYNDROME. 7th International Myology Congress, 2022, Nice, France. ⟨hal-04002800⟩
  • Tomoya Kubota, Fenfen Wu, Savine Vicart, Maki Nakaza, Damien Sternberg, et al.. Hypokalaemic periodic paralysis with a charge-retaining substitution in the voltage sensor. Brain Communications, 2021, 2 (2), ⟨10.1093/braincomms/fcaa103⟩. ⟨hal-03464510⟩
Assistance Publique Hôpitaux de Paris
Fondation de l'avenir - Accélérateur de progrès médical
Association pour la recherche sur la SLA
Satt Lutech
Inserm Transfert
AMO Pharma

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