Remyelination, namely, the formation of new myelin sheaths around denuded axons, counteracts axonal degeneration and restores neuronal function. Considerable advances have been made in understanding this regenerative process that often fails in diseases like multiple sclerosis, leaving axons demyelinated and vulnerable to damage, thus contributing to disease progression. The identification of the membrane receptor GPR17 on a subset of oligodendrocyte precursor cells (OPCs), which mediate remyelination in the adult central nervous system (CNS), has led to a huge amount of evidence that validated this receptor as a new attractive target for remyelinating therapies. Here, we summarize the role of GPR17 in OPC function, myelination and remyelination, describing its atypical pharmacology, its downstream signaling, and the genetic and epigenetic factors modulating its activity. We also highlight crucial insights into GPR17 pathophysiology coming from the demonstration that oligodendrocyte injury, associated with inflammation in chronic neurodegenerative conditions, is invariably characterized by abnormal and persistent GPR17 upregulation, which, in turn, is accompanied by a block of OPCs at immature premyelinating stages. Finally, we discuss the current literature in light of the potential exploitment of GPR17 as a therapeutic target to promote remyelination.

Regulation and signaling of the GPR17 receptor in oligodendroglial cells / D. Lecca, S. Raffaele, M.P. Abbracchio, M. Fumagalli. - In: GLIA. - ISSN 0894-1491. - 68:10(2020 Oct), pp. 1957-1967. [10.1002/glia.23807]

Regulation and signaling of the GPR17 receptor in oligodendroglial cells

D. Lecca
Primo
;
S. Raffaele
Secondo
;
M.P. Abbracchio
Penultimo
;
M. Fumagalli
Ultimo
2020

Abstract

Remyelination, namely, the formation of new myelin sheaths around denuded axons, counteracts axonal degeneration and restores neuronal function. Considerable advances have been made in understanding this regenerative process that often fails in diseases like multiple sclerosis, leaving axons demyelinated and vulnerable to damage, thus contributing to disease progression. The identification of the membrane receptor GPR17 on a subset of oligodendrocyte precursor cells (OPCs), which mediate remyelination in the adult central nervous system (CNS), has led to a huge amount of evidence that validated this receptor as a new attractive target for remyelinating therapies. Here, we summarize the role of GPR17 in OPC function, myelination and remyelination, describing its atypical pharmacology, its downstream signaling, and the genetic and epigenetic factors modulating its activity. We also highlight crucial insights into GPR17 pathophysiology coming from the demonstration that oligodendrocyte injury, associated with inflammation in chronic neurodegenerative conditions, is invariably characterized by abnormal and persistent GPR17 upregulation, which, in turn, is accompanied by a block of OPCs at immature premyelinating stages. Finally, we discuss the current literature in light of the potential exploitment of GPR17 as a therapeutic target to promote remyelination.
No
English
GPR17; neuroinflammatory diseases; oligodendrocyte progenitors; remyelination; signal transduction
Settore BIO/14 - Farmacologia
Review essay
Esperti anonimi
Pubblicazione scientifica
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ott-2020
22-feb-2020
Wiley Blackwell Publishing
68
10
1957
1967
11
Pubblicato
Periodico con rilevanza internazionale
pubmed
Aderisco
info:eu-repo/semantics/article
Regulation and signaling of the GPR17 receptor in oligodendroglial cells / D. Lecca, S. Raffaele, M.P. Abbracchio, M. Fumagalli. - In: GLIA. - ISSN 0894-1491. - 68:10(2020 Oct), pp. 1957-1967. [10.1002/glia.23807]
partially_open
Prodotti della ricerca::01 - Articolo su periodico
4
262
Article (author)
Periodico con Impact Factor
D. Lecca, S. Raffaele, M.P. Abbracchio, M. Fumagalli
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/753340
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