High-Affinity Zn Block in Recombinant N-Methyl-D-Aspartate Receptors with Cysteine Substitutions at the Q/R/N Site

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High-Affinity Zn Block in Recombinant N-Methyl-D-Aspartate Receptors with Cysteine Substitutions at the Q/R/N Site

Muriel Amar, Florent Perin-Dureau, and Jacques Neyton

Laboratoire de Neurobiologie, Ecole Normale Supérieure, 75005 Paris, France

In ionotropic glutamate receptors, many channel properties (e.g., selectivity, ion permeation, and ion block) depend on theresidue (glutamine, arginine, or asparagine) located at the tipof the pore loop (the Q/R/N site). We substituted a cysteine forthe asparagine present at that position in both NR1 and NR2 N-methyl-D-aspartate(NMDA) receptor subunits. Under control conditions, receptorscontaining mutated NR1 and NR2 subunits show much smaller glutamateresponses than wild-type receptors. However, this difference disappearsupon addition of heavy metal chelators in the extracellular bath.The presence of cysteines at the Q/R/N site in both subunits ofNR1/NR2C receptors results in a 220,000-fold increase in sensitivityof the inhibition by extracellular Zn. In contrast with the high-affinityZn inhibition of wild-type NR1/NR2A receptors, the high-affinityZn inhibition of mutated NR1/NR2C receptors shows a voltage dependence,which resembles very much that of the block by extracellular Mg.This indicates that the Zn inhibition of the mutated receptorsresults from a channel block involving Zn binding to the thiolgroups introduced into the selectivity filter. Taking advantageof the slow kinetics of the Zn block, we show that both blockingand unblocking reactions require prior opening of thechannel.

Biophys J, July 2001, p. 107-116, Vol. 81, No. 1
© 2001 by the Biophysical Society 0006-3495/01/07/107/10 $2.00

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