A TEAM OF RESEARCHERS LED BY BRAHIM NAIT OUMESMAR, INSERM RESEARCH DIRECTOR AT THE PITIE-SALPETRIERE NEUROSCIENCES RESEARCH CENTER (CRICM) IN COLLABORATION WITH THE UNIVERSITY OF LUXEMBOURG,

HAS JUST DISCOVERED A NEW MOLECULE CAPABLE OF STIMULATING THE REPAIR OF THE MYELIN DESTROYED IN EXPERIMENTAL MODELS OF MULTIPLE SCLEROSIS. THIS ADVANCE WILL BE PUBLISHED IN _THE JOURNAL OF

NEUROSCIENCE._ Multiple Sclerosis (MS) is the most frequent cause of disability in young adults [1]. The condition is characterised by inflammatory lesions in the brain, spinal cord and

optic nerve. It is considered to be an auto-immune disease. In MS sufferers, the defence system becomes disordered. Instead of fighting external pathogens, the immune system attacks its own

designed to stimulate remyelinisation is thus a major new research direction for MS. Remyelinisation might make it possible to re-establish nerve conduction and prevent the condition of MS

sufferers from deteriorating further. The research team headed by Brahim Nait Oumesmar, Inserm research director at the PITIE-SALPETRIERE NEUROSCIENCES RESEARCH CENTER (CRICM) in

collaboration with the University of Luxembourg, has identified a new synthesising molecule capable of stimulating the repair of myelin lesions in experimental models of MS. This synthesis

molecule, known as TFA-12, is part of a derivative of vitamin E. Their work has shown that TFA-12 both reduces the formation of inflammatory lesions but, above all, favours the repair of

myelin lesions. Research has also shown that this molecule stimulates the regeneration of the oligodendrocytes, the cells that are the origin of myelin synthesis in the central nervous

system.  This work will thus enable the development of new pharmacological strategies, promoting the remyelinisation of the neurons in cases of MS. [1] The average age at which the symptoms

first appear is thirty, and the condition affects more women than men. There are 80,000 MS sufferers in France. THESE CONTENTS COULD BE INTERESTING :