However, taking into consideration lipid binding to recombinant C terminal P2X2 channel constructs, they www.selleckchem.com/products/Bosutinib.html proposed that PI P and PI P2, rather than PIP2 or PIP3, are the main regulators of homomeric P2X2 function. Likely Inhibitors,Modulators,Libraries due to less stringent experimental conditions, we show a significant binding of the C terminus of P2X2 to PIP2 and PIP3, as well as many other anionic phospholipids. Sensitivity of P2X3 Inhibitors,Modulators,Libraries current to PIP2 depletion in HEK293 cells is reversed by R356Q mutation Phospholipid modulation of P2X3 receptors does not involve direct binding Several groups have reported the direct binding of the P2X receptors to phospholipid containing membranes, using a biochemical approach in which GST fusion proteins of various P2X C terminal domains suspected to mediate the binding were tested on lipid strips.
To test if P2X3 modulation involved direct binding to phosphoi nositides, GST fusion proteins coding for the C terminal region of P2X3 homologous to the identified phosphoi nositide binding region in other P2X receptors were gen erated. The C terminus was a candidate domain as it has been shown to be Inhibitors,Modulators,Libraries involved in the modulatory function of several P2X receptor channels, most notably their desensi tization and membrane targeting. Sur prisingly, no binding of the recombinant P2X3 constructs to any phospholipids could be detected above back ground. The N terminus of the Kir channel family has been shown to interact with PIP2for their gating modula tion. This led us to test the possibility that interaction between the P2X3 receptor and PIP2 involved its N termi nal domain.
Again, no such interaction was observed as the binding of N terminal P2X3 constructs to phospholi pid membranes was not detected. Therefore P2X3 is the only member of the P2X family, so far, that does not dis play direct binding to phosphoinositides using the lipid strip assay. Inhibitors,Modulators,Libraries We cannot rule out, however, the possibility that phosphoinositide binding requires the intact P2X3 receptor subunit. Indirect modulation of ion channels by phosphoi nositides is not ungrounded. For instance, Inhibitors,Modulators,Libraries Michailidis and coll. have recently shown that the regulation of the NMDA receptor by PIP2 requires the intracellular protein actinin, which serves as a partner of NMDAR2 subunit facilitating phospholipid sensing. Moreover, Kim and coll.
have reported a novel protein called PIRT, expressed in nociceptive neurons of DRG, which binds to TRPV1 channels and several phosphoinositides, including PIP2, to modulate TRPV1 activity. Overall, the require ment of a specific partner protein currently mediating the interac tion between phosphoinositides and the P2X3 subunit may explain why the modulatory effects of phosphoi nositides on P2X3 receptors seen in DRG neurons was not observed in HEK293 cells. The expression of a potential lipid binding protein linked to P2X3 subunits remains to be investigated in DRG neurons.