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Phylogeny of proteolipid proteins: divergence, constraints, and the evolution of novel functions in myelination and neuroprotection

Journal

NEURON GLIA BIOLOGY
Volume 4, Issue -, Pages 111-127

Publisher

CAMBRIDGE UNIV PRESS
DOI: 10.1017/S1740925X0900009X

Keywords

Myelin; oligodendrocyte; Schmidt-Lanterman incisure; Pelizaeus-Merzbacher disease; spastic paraplegia; neurite outgrowth; PLP/DM20; M6; OSP/claudin-11; Po/MPZ

Categories

Funding

  1. BMBF (DLR-Leukonet)

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The protein composition of myelin in the central nervous system (CNS) has changed at the evolutionary transition from fish to tetrapods, when a lipid-associated transmembrane-tetraspan (proteolipid protein, PLP) replaced an adhesion protein of the immunoglobulin superfamily (Po) as the most abundant constituent. Here, we review major steps of proteolipid evolution. Three paralog proteolipids (PLP/DM2o/DM alpha, M6B/DM gamma and the neuronal glycoprotein M6A/DM beta) exist in vertebrates from cartilaginous fish to mammals and one (M6/CG7540) can be traced in invertebrate bilaterians including the planktonic copepod Calanus finmarchicus that possess a functional myelin equivalent. In fish, DM alpha and DM gamma are coexpressed in oligodendrocytes but are not major myelin components. PLP emerged at the root of tetrapods by the acquisition Of an enlarged cytoplasmic loop in the evolutionary older DM alpha/DM20. Transgenic experiments in mice suggest that this loop enhances the incorporation of PLP into myelin. The evolutionary recruitment of PLP as the major myelin protein provided oligodendrocytes with the competence to support long-term axonal integrity. We suggest that the molecular shift from Po to PLP also correlates with the concentration of adhesive forces at the radial component, and that the new balance between membrane adhesion and dynamics was favorable for CNS myelination.

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