@article{9cdce156da96481fa70211800e21ef6d,
title = "The dual PDZ domain from Postsynaptic density protein 95 forms a scaffold with peptide ligand",
abstract = "PSD-95 is a member of the membrane-associated guanylate kinase class of proteins that forms scaffolding interactions with partner proteins, including ion and receptor channels. PSD-95 is directly implicated in modulating the electrical responses of excitable cells. The first two PSD-95/disks large/zona occludens (PDZ) domains of PSD-95 have been shown to be the key component in the formation of channel clusters. We report crystal structures of this dual domain in both apo- and ligand-bound form: thermodynamic analysis of the ligand association and small-angle x-ray scattering of the dual domain in the absence and presence of ligands. These experiments reveal that the ligated double domain forms a three-dimensional scaffold that can be described by a space group. The concentration of the components in this study is comparable with those found in compartments of excitable cells such as the postsynaptic density and juxtaparanodes of Ranvier. These in vitro experiments inform the basis of the scaffolding function of PSD-95 and provide a detailed model for scaffold formation by the PDZ domains of PSD-95.",
keywords = "protein-protein interaction, biophysical analysis, clustering, PDZ domain, MAGUK, scaffold protein",
author = "Nazahiyah Rodzli and Michael Lockhart and Levy, {C W} and J Chipperfield and L Bird and Clair Baldock and Prince, {Stephen M.}",
note = "Funding Information: X-ray crystallographic data were collected at Diamond Light Source Beamlines I04 and I04-1. ITC was conducted in the Biophysical Analysis Core Facility of the University of Manchester. SAXS data were collected at the DESY Synchrotron Beamline P21 and at Diamond Light Source Beamline B21. N.A.R. was supported by a Majlis Amanah Rakyat Malaysian Government Scholarship. J.C. was supported by a BBSRC/EPSRC Doctoral Training award. C.B. and M.P.L.-C. are members of the Wellcome Trust Centre for Cell-Matrix Research, which is supported by funding from the Wellcome Trust ( 203128/Z/16/Z ). C.B. gratefully acknowledges BBSRC funding ( BB/N015398/1 and BB/R008221/1 ). Funding Information: X-ray crystallographic data were collected at Diamond Light Source Beamlines I04 and I04-1. ITC was conducted in the Biophysical Analysis Core Facility of the University of Manchester. SAXS data were collected at the DESY Synchrotron Beamline P21 and at Diamond Light Source Beamline B21. N.A.R. was supported by a Majlis Amanah Rakyat Malaysian Government Scholarship. J.C. was supported by a BBSRC/EPSRC Doctoral Training award. C.B. and M.P.L.-C. are members of the Wellcome Trust Centre for Cell-Matrix Research, which is supported by funding from the Wellcome Trust (203128/Z/16/Z). C.B. gratefully acknowledges BBSRC funding (BB/N015398/1 and BB/R008221/1). Publisher Copyright: {\textcopyright} 2020 Biophysical Society",
year = "2020",
month = aug,
day = "4",
doi = "10.1016/j.bpj.2020.06.018",
language = "English",
volume = "119",
pages = "667--689",
journal = "Biophysical Journal",
issn = "0006-3495",
publisher = "Cell Press",
number = "3",
}