TREM2 activation on microglia promotes myelin debris clearance and remyelination in a model of multiple sclerosis

Francesca Cignarella; Fabia Filipello; Bryan Bollman; Claudia Cantoni; Alberto Locca; Robert Mikesell; Melissa Manis; Adiljan Ibrahim; Li Deng; Bruno A. Benítez; Carlos Cruchaga; Danilo Licastro; Kathie A. Mihindukulasuriya; Oscar Harari; Michael E. Buckland; David M. Holtzman; Arnon Rosenthal; Tina Schwabe; Ilaria Tassi; Laura Piccio

doi:10.1007/s00401-020-02193-z

TREM2 activation on microglia promotes myelin debris clearance and remyelination in a model of multiple sclerosis

Francesca Cignarella(Washington University in St. Louis), Fabia Filipello(Humanitas University), Bryan Bollman(Washington University in St. Louis), Claudia Cantoni(Washington University in St. Louis), Alberto Locca(Washington University in St. Louis), Robert Mikesell(Washington University in St. Louis), Melissa Manis(Washington University in St. Louis), Adiljan Ibrahim(Alector (United States)), Li Deng(Washington University in St. Louis), Bruno A. Benítez(Washington University in St. Louis), Carlos Cruchaga(Washington University in St. Louis), Danilo Licastro(AREA Science Park), Kathie A. Mihindukulasuriya(Washington University in St. Louis), Oscar Harari(Washington University in St. Louis), Michael E. Buckland(The University of Sydney), David M. Holtzman(Washington University in St. Louis), Arnon Rosenthal(Alector (United States)), Tina Schwabe(Alector (United States)), Ilaria Tassi(Alector (United States)), Laura Piccio(The University of Sydney)

Acta Neuropathologica

August 9, 2020

10.1007/s00401-020-02193-z

Cited by 375Open Access

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Abstract

Multiple sclerosis (MS) is an inflammatory, demyelinating, and neurodegenerative disease of the central nervous system (CNS) triggered by autoimmune mechanisms. Microglia are critical for the clearance of myelin debris in areas of demyelination, a key step to allow remyelination. TREM2 is expressed by microglia and promotes microglial survival, proliferation, and phagocytic activity. Herein we demonstrate that TREM2 was highly expressed on myelin-laden phagocytes in active demyelinating lesions in the CNS of subjects with MS. In gene expression studies, macrophages from subjects with TREM2 genetic deficiency displayed a defect in phagocytic pathways. Treatment with a new TREM2 agonistic antibody promoted the clearance of myelin debris in the cuprizone model of CNS demyelination. Effects included enhancement of myelin uptake and degradation, resulting in accelerated myelin debris removal by microglia. Most importantly, antibody-dependent TREM2 activation on microglia increased density of oligodendrocyte precursors in areas of demyelination, as well as the formation of mature oligodendrocytes thus enhancing remyelination and axonal integrity. These results are relevant as they propose TREM2 on microglia as a potential new target to promote remyelination.

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