Background: The P2X7 receptor is present in a variety of cell types involved in pain, inflammatory processes and neurodegenerative conditions, thus it may be an appealing target for pharmacological intervention. The extensive use of high-throughput screening (HTS) followed by a hit-to-lead (HtL) program, has prompted a number of firms to identify highly selective and metabolically stable small-molecules possessing activity for both the rat and human P2X7 receptor, which provide a novel therapeutic approach to the treatment of pain as well as neurodegenerative and inflammatory disorders. Objective: To describe the current status of and potential for development of P2X7 receptor-antagonists. Methods: A literature review. Results/conclusions: We describe the recent discoveries of novel P2X7 receptor-selective antagonists, along with their biological activity and therapeutic potential.

The P2X7 receptor as a therapeutic target.

ROMAGNOLI, Romeo;BARALDI, Pier Giovanni;PRETI, Delia;BOREA, Pier Andrea;GESSI, Stefania
2008

Abstract

Background: The P2X7 receptor is present in a variety of cell types involved in pain, inflammatory processes and neurodegenerative conditions, thus it may be an appealing target for pharmacological intervention. The extensive use of high-throughput screening (HTS) followed by a hit-to-lead (HtL) program, has prompted a number of firms to identify highly selective and metabolically stable small-molecules possessing activity for both the rat and human P2X7 receptor, which provide a novel therapeutic approach to the treatment of pain as well as neurodegenerative and inflammatory disorders. Objective: To describe the current status of and potential for development of P2X7 receptor-antagonists. Methods: A literature review. Results/conclusions: We describe the recent discoveries of novel P2X7 receptor-selective antagonists, along with their biological activity and therapeutic potential.
2008
Romagnoli, Romeo; Baraldi, Pier Giovanni; CRUZ LOPEZ, O; LOPEZ CARA, C; Preti, Delia; Borea, Pier Andrea; Gessi, Stefania
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11392/529811
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