Molecular cloning, functional characterization and possible cooperativity between the murine P2X4 and P2X4a receptors

Townsend-Nicholson, Andrea, King, Brian F., Wildman, Scott S. and Burnstock, Geoffrey (1999) Molecular cloning, functional characterization and possible cooperativity between the murine P2X4 and P2X4a receptors. Molecular Brain Research, 64 (2). pp. 246-254. ISSN 0169328X

Abstract

We have cloned and functionally characterised the mouse orthologue of the P2X4 receptor, mP2X4, and a splice variant of this receptor, mP2X4a. mP2X4 is 388 amino acids in length and shares 94% and 87% identity with the rat and human P2X4 receptors, respectively, while mP2X4a is 361 amino acids in length and lacks a 27-amino acid region in the extracellular domain corresponding to exon 6 of the known P2X receptor gene structures. When expressed in Xenopus laevis oocytes, mP2X4 produces a rapid inward current in response to ATP with an EC50 of 1.68+/-0.2 microM, consistent with the affinity of the rat and human P2X4 receptors for ATP. This agonist response is potentiated by the P2X receptor antagonists suramin, Reactive blue 2 and, over a limited concentration range, by PPADS. Although mP2X4a forms a poorly functional homomeric receptor, it appears able to interact with the full-length mP2X4 subunit to result in a functional channel with a reduced affinity for ATP. These results suggest a possible role for splice variants of P2X receptors in the formation of functional heteromeric ion channels.

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Official URL:	https://doi.org/10.1016/s0169-328x(98)00328-3
Item Type:	Article
Disciplines:	?? Biology ??
Depositing User:	Saxony Anders
Date Deposited:	12 Jul 2023 09:22
Last Modified:	16 Jan 2024 10:33
URI:	https://nul.repository.guildhe.ac.uk/id/eprint/98

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