PDBsum entry 2zpy

Cell adhesion

PDB id

2zpy

Loading ...

Contents

			Protein chain

					295 a.a. *

			Ligands

					GLN-LYS-LYS-LYS- LEU-VAL-ILE-ASN- GLY

			Waters ×171

* Residue conservation analysis

PDB id:

2zpy

Links

Name:

Cell adhesion

Title:

Crystal structure of the mouse radxin ferm domain complexed with the mouse cd44 cytoplasmic peptide

Structure:

Radixin. Chain: a. Fragment: ferm domain (residues 1-310). Synonym: esp10. Engineered: yes. Cd44 antigen. Chain: b. Fragment: residues 293-312. Engineered: yes

Source:

Mus musculus. Mouse. Organism_taxid: 10090. Gene: rdx. Expressed in: escherichia coli. Expression_system_taxid: 562. Synthetic: yes. Other_details: peptide synthesis

Resolution:

2.10Å

R-factor:

0.231

R-free:

0.256

Authors:

T.Mori,K.Kitano,S.Terawaki,R.Maesaki,Y.Fukami,T.Hakoshima

Key ref:

T.Mori et al. (2008). Structural basis for CD44 recognition by ERM proteins. J Biol Chem, 283, 29602-29612. PubMed id: 18753140 DOI: 10.1074/jbc.M803606200

Date:

31-Jul-08

Release date:

26-Aug-08

PROCHECK

	Headers

	References

Protein chain

P26043 (RADI_MOUSE) - Radixin from Mus musculus

Seq: Struc:

Seq: Struc:					583 a.a. 295 a.a.

Key:

PfamA domain

Secondary structure

CATH domain

DOI no: 10.1074/jbc.M803606200	J Biol Chem 283:29602-29612 (2008)
PubMed id: 18753140

Structural basis for CD44 recognition by ERM proteins.
T.Mori, K.Kitano, S.Terawaki, R.Maesaki, Y.Fukami, T.Hakoshima.

ABSTRACT

CD44 is an important adhesion molecule that functions as the major hyaluronan receptor which mediates cell adhesion and migration in a variety of physiological and pathological processes. Although full activity of CD44 requires binding to ERM (ezrin/radixin/moesin) proteins, the CD44 cytoplasmic region, consisting of 72 amino acid residues, lacks the Motif-1 consensus sequence for ERM binding found in intercellular adhesion molecule (ICAM)-2 and other adhesion molecules of the immunoglobulin superfamily. Ultracentrifugation sedimentation studies and circular dichroism measurements revealed an extended monomeric form of the cytoplasmic peptide in solution. The crystal structure of the radixin FERM domain complexed with a CD44 cytoplasmic peptide reveals that the KKKLVIN sequence of the peptide forms a beta strand followed by a short loop structure that binds subdomain C of the FERM domain. Like Motif-1 binding, the CD44 beta strand binds the shallow groove between strand beta5C and helix alpha1C and augments the beta sheet beta5C-beta7C from subdomain C. Two hydrophobic CD44 residues, Leu and Ile, are docked into a hydrophobic pocket with the formation of hydrogen bonds between Asn of the CD44 short loop and loop beta4C-beta5C from subdomain C. This binding mode resembles that of NEP (neutral endopeptidase 24.11) rather than ICAM-2. Our results reveal a characteristic versatility of peptide recognition by the FERM domains from ERM proteins, suggest a possible mechanism by which the CD44 tail is released from the cytoskeleton for nuclear translocation by regulated intramembrane proteolysis, and provide a structural basis for Smad1 interactions with activated CD44 bound to ERM protein.

Selected figure(s)



	Figure 2. Crystal structure of the FERM-CD44 complex. A, ribbon representations of the radixin FERM domain complexed with the CD44 cytoplasmic peptide (blue). The radixin FERM domain comprises three subdomains: A (residues 3-82 in green), B (residues 96-195 in red), and C (residues 204-297 in yellow). Linkers A-B (residues 83-95) and B-C (residues 196-203) are colored gray. B, surface electrostatic potentials of the FERM domain and a close-up view of the CD44 cytoplasmic peptide docked into the groove formed between helix α1C and strand β5C of subdomain C. The peptide is shown as a stick model (labeled with one-letter codes), and the four side chain-binding sites (S1--S4) for the bound β strand of CD44 and the deep hydrophobic pocket (P1) are labeled and indicated with yellow dashed circles. Site S4 adjoins pocket P1. C, a stick model of the CD44 cytoplasmic peptide is shown in the omit electron density map for the CD44 cytoplasmic peptide at the contour level of 1σ.		Figure 4. Comparison of ICAM-2, NEP, and CD44 peptides bound to the FERM domain. Shown is superposition of ICAM-2 (magenta) from the FERM-ICAM-2 complex (28) and NEP (green) from the FERM-NEP complex (31) on the FERM-CD44 complex. The N-terminal extensions of ICAM-2 and CD44 or the C terminus of NEP that would be linked to the transmembrane helix in the plasmamembrane are indicated with dotted lines.

Figures were selected by an automated process.

Literature references that cite this PDB file's key reference

PubMed id

Reference

21258793

M.K.Hertweck, F.Erdfelder, and K.A.Kreuzer (2011).
CD44 in hematological neoplasias.

Ann Hematol, 90, 493-508.

21390059

M.Zöller (2011).
CD44: can a cancer-initiating cell profit from an abundantly expressed molecule?

Nat Rev Cancer, 11, 254-267.

21321230

Z.Wei, J.Yan, Q.Lu, L.Pan, and M.Zhang (2011).
Cargo recognition mechanism of myosin X revealed by the structure of its tail MyTH4-FERM tandem in complex with the DCC P3 domain.

Proc Natl Acad Sci U S A, 108, 3572-3577.

PDB code:

3pzd

20565253

J.R.Couchman (2010).
Transmembrane signaling proteoglycans.

Annu Rev Cell Dev Biol, 26, 89.

20178130

N.Takahashi, C.B.Knudson, S.Thankamony, W.Ariyoshi, L.Mellor, H.J.Im, and W.Knudson (2010).
Induction of CD44 cleavage in articular chondrocytes.

Arthritis Rheum, 62, 1338-1348.

19913036

Q.Xu, A.Bateman, R.D.Finn, P.Abdubek, T.Astakhova, H.L.Axelrod, C.Bakolitsa, D.Carlton, C.Chen, H.J.Chiu, M.Chiu, T.Clayton, D.Das, M.C.Deller, L.Duan, K.Ellrott, D.Ernst, C.L.Farr, J.Feuerhelm, J.C.Grant, A.Grzechnik, G.W.Han, L.Jaroszewski, K.K.Jin, H.E.Klock, M.W.Knuth, P.Kozbial, S.S.Krishna, A.Kumar, D.Marciano, D.McMullan, M.D.Miller, A.T.Morse, E.Nigoghossian, A.Nopakun, L.Okach, C.Puckett, R.Reyes, C.L.Rife, N.Sefcovic, H.J.Tien, C.B.Trame, H.van den Bedem, D.Weekes, T.Wooten, K.O.Hodgson, J.Wooley, M.A.Elsliger, A.M.Deacon, A.Godzik, S.A.Lesley, and I.A.Wilson (2010).
Bacterial pleckstrin homology domains: a prokaryotic origin for the PH domain.

J Mol Biol, 396, 31-46.

PDB codes:

3b77 3dcx 3hsa

19884346

R.F.Hennigan, L.A.Foster, M.F.Chaiken, T.Mani, M.M.Gomes, A.B.Herr, and W.Ip (2010).
Fluorescence resonance energy transfer analysis of merlin conformational changes.

Mol Cell Biol, 30, 54-67.

20308985

R.G.Fehon, A.I.McClatchey, and A.Bretscher (2010).
Organizing the cell cortex: the role of ERM proteins.

Nat Rev Mol Cell Biol, 11, 276-287.

20017116

R.L.Rich, and D.G.Myszka (2010).
Grading the commercial optical biosensor literature-Class of 2008: 'The Mighty Binders'.

J Mol Recognit, 23, 1.

19893486

S.Terawaki, K.Kitano, T.Mori, Y.Zhai, Y.Higuchi, N.Itoh, T.Watanabe, K.Kaibuchi, and T.Hakoshima (2010).
The PHCCEx domain of Tiam1/2 is a novel protein- and membrane-binding module.

EMBO J, 29, 236-250.

PDB codes:

3a8n 3a8p 3a8q

19783662

C.Duterme, J.Mertens-Strijthagen, M.Tammi, and B.Flamion (2009).
Two novel functions of hyaluronidase-2 (Hyal2) are formation of the glycocalyx and control of CD44-ERM interactions.

J Biol Chem, 284, 33495-33508.

19388049

M.Y.Niv, K.Iida, R.Zheng, A.Horiguchi, R.Shen, and D.M.Nanus (2009).
Rational redesign of neutral endopeptidase binding to merlin and moesin proteins.

Protein Sci, 18, 1042-1050.

19195913

R.A.Andhare, N.Takahashi, W.Knudson, and C.B.Knudson (2009).
Hyaluronan promotes the chondrocyte response to BMP-7.

Osteoarthritis Cartilage, 17, 906-916.

19596566

U.Tepass (2009).
FERM proteins in animal morphogenesis.

Curr Opin Genet Dev, 19, 357-367.

The most recent references are shown first. Citation data come partly from CiteXplore and partly from an automated harvesting procedure. Note that this is likely to be only a partial list as not all journals are covered by either method. However, we are continually building up the citation data so more and more references will be included with time. Where a reference describes a PDB structure, the PDB code is shown on the right.