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. 1997 May;18(5):803-14.
doi: 10.1016/s0896-6273(00)80319-0.

Disulfide-linked head-to-head multimerization in the mechanism of ion channel clustering by PSD-95

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Disulfide-linked head-to-head multimerization in the mechanism of ion channel clustering by PSD-95

Y P Hsueh et al. Neuron. 1997 May.
Free article

Abstract

The PSD-95/SAP90 family of PDZ-containing proteins is directly involved in the clustering of specific ion channels at synapses. We report that channel clustering depends on a conserved N-terminal domain of PSD-95 that mediates multimerization and disulfide linkage of PSD-95 protomers. This N-terminal multimerization domain confers channel clustering activity on a single PDZ domain. Thus, channel clustering depends on aggregation of PDZ domains achieved by head-to-head multimerization of PSD-95, rather than by concatenation of PDZ domains in PSD-95 monomers. This mechanism predicts that PSD-95 can organize heterogeneous membrane protein clusters via differential binding specificities of its three PDZ domains. PSD-95 and its relative chapsyn-110 exist as disulfide-linked complexes in rat brain, consistent with head-to-head multimerization of these proteins in vivo.

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