The PDZ Domain of Human Erythrocyte P55 Mediates Its Binding to the Cytoplasmic Carboxyl Terminus of Glycophorin C. Analysis of the Binding Interface by in Vitro Mutagenesis

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 1997 Sep 26

PMID 9305870

Citations 17

Authors

S M Marfatia

A C Kim

O Byron

A H Chishti

Affiliations

Soon will be listed here.

Abstract

The PDZ domain, also known as the GLGF repeat/DHR domain, is an approximately 90-amino acid motif discovered in a recently identified family of proteins termed MAGUKs (membrane-associated guanylate kinase homologues). Sequence comparison analysis has since identified PDZ domains in over 50 proteins. Like SH2 and SH3 domains, the PDZ domains mediate specific protein-protein interactions, whose specificities appear to be dictated by the primary structure of the PDZ domain as well as its binding target. Using recombinant fusion proteins and a blot overlay assay, we show that a single copy of the PDZ domain in human erythrocyte p55 binds to the carboxyl terminus of the cytoplasmic domain of human erythroid glycophorin C. Deletion mutagenesis of 21 amino acids at the amino terminus of the p55 PDZ domain completely abrogates its binding activity for glycophorin C. Using an alanine scan and surface plasmon resonance technique, we identify residues in the cytoplasmic domain of glycophorin C that are critical for its interaction with the PDZ domain. The recognition specificity of the p55 PDZ domain appears to be unique, since the three PDZ domains of hDlg (human lymphocyte homologue of the Drosophila discs large tumor suppressor) do not bind the cytoplasmic domain of glycophorin C. Taken together with our previous studies, these results complete the identification of interacting domains in the ternary complex between p55, glycophorin C, and protein 4.1. Implications of these findings are discussed in terms of binding specificity and the regulation of cytoskeleton-membrane interactions.

Citing Articles

Molecular characterization of direct interactions between MPP1 and flotillins.

Biernatowska A, Olszewska P, Grzymajlo K, Drabik D, Kraszewski S, Sikorski A Sci Rep. 2021; 11(1):14751.

PMID: 34285255 PMC: 8292550. DOI: 10.1038/s41598-021-93982-3.

Not Just Another Scaffolding Protein Family: The Multifaceted MPPs.

Chytla A, Gajdzik-Nowak W, Olszewska P, Biernatowska A, Sikorski A, Czogalla A Molecules. 2020; 25(21).

PMID: 33114686 PMC: 7662862. DOI: 10.3390/molecules25214954.

An unexpected protein interaction promotes drug resistance in leukemia.

Pitre A, Ge Y, Lin W, Wang Y, Fukuda Y, Temirov J Nat Commun. 2017; 8(1):1547.

PMID: 29146910 PMC: 5691054. DOI: 10.1038/s41467-017-01678-y.

Protein distribution during human erythroblast enucleation in vitro.

Bell A, Satchwell T, Heesom K, Hawley B, Kupzig S, Hazell M PLoS One. 2013; 8(4):e60300.

PMID: 23565219 PMC: 3614867. DOI: 10.1371/journal.pone.0060300.

Characterization of cytoskeletal protein 4.1R interaction with NHE1 (Na(+)/H(+) exchanger isoform 1).

Nunomura W, Denker S, Barber D, Takakuwa Y, Gascard P Biochem J. 2012; 446(3):427-35.

PMID: 22731252 PMC: 4338608. DOI: 10.1042/BJ20120535.