Protein tyrosine phosphatases: Structure-function relationships

Lydia Tabernero; A. Radu Aricescu; E. Yvonne Jones; Stefan E. Szedlacsek

doi:10.1111/j.1742-4658.2008.06251.x

Protein tyrosine phosphatases: Structure-function relationships

Lydia Tabernero, A. Radu Aricescu, E. Yvonne Jones, Stefan E. Szedlacsek

Research output: Contribution to journal › Article › peer-review

Abstract

Structural analysis of protein tyrosine phosphatases (PTPs) has expanded considerably in the last several years, producing more than 200 structures in this class of enzymes (from 35 different proteins and their complexes with ligands). The small-medium size of the catalytic domain of ∼280 residues plus a very compact fold makes it amenable to cloning and overexpression in bacterial systems thus facilitating crystallographic analysis. The low molecular weight PTPs being even smaller, ∼150 residues, are also perfect targets for NMR analysis. The availability of different structures and complexes of PTPs with substrates and inhibitors has provided a wealth of information with profound effects in the way we understand their biological functions. Developments in mammalian expression technology recently led to the first crystal structure of a receptor-like PTP extracellular region. Altogether, the PTP structural work significantly advanced our knowledge regarding the architecture, regulation and substrate specificity of these enzymes. In this review, we compile the most prominent structural traits that characterize PTPs and their complexes with ligands. We discuss how the data can be used to design further functional experiments and as a basis for drug design given that many PTPs are now considered strategic therapeutic targets for human diseases such as diabetes and cancer. © 2008 The Authors.

Original language	English
Pages (from-to)	867-882
Number of pages	15
Journal	FEBS Journal
Volume	275
Issue number	5
DOIs	https://doi.org/10.1111/j.1742-4658.2008.06251.x
Publication status	Published - Mar 2008

Keywords

Catalytic mechanism
Cell adhesion
Cell signalling
Drug design
Ligand binding
NMR
Phosphatase inhibitor
Protein structure
Protein tyrosine phosphatase
Structure-function receptor
X-ray crystallography

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1111/j.1742-4658.2008.06251.x

Cite this

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title = "Protein tyrosine phosphatases: Structure-function relationships",

abstract = "Structural analysis of protein tyrosine phosphatases (PTPs) has expanded considerably in the last several years, producing more than 200 structures in this class of enzymes (from 35 different proteins and their complexes with ligands). The small-medium size of the catalytic domain of ∼280 residues plus a very compact fold makes it amenable to cloning and overexpression in bacterial systems thus facilitating crystallographic analysis. The low molecular weight PTPs being even smaller, ∼150 residues, are also perfect targets for NMR analysis. The availability of different structures and complexes of PTPs with substrates and inhibitors has provided a wealth of information with profound effects in the way we understand their biological functions. Developments in mammalian expression technology recently led to the first crystal structure of a receptor-like PTP extracellular region. Altogether, the PTP structural work significantly advanced our knowledge regarding the architecture, regulation and substrate specificity of these enzymes. In this review, we compile the most prominent structural traits that characterize PTPs and their complexes with ligands. We discuss how the data can be used to design further functional experiments and as a basis for drug design given that many PTPs are now considered strategic therapeutic targets for human diseases such as diabetes and cancer. {\textcopyright} 2008 The Authors.",

keywords = "Catalytic mechanism, Cell adhesion, Cell signalling, Drug design, Ligand binding, NMR, Phosphatase inhibitor, Protein structure, Protein tyrosine phosphatase, Structure-function receptor, X-ray crystallography",

author = "Lydia Tabernero and Aricescu, {A. Radu} and Jones, {E. Yvonne} and Szedlacsek, {Stefan E.}",

year = "2008",

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doi = "10.1111/j.1742-4658.2008.06251.x",

language = "English",

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AU - Aricescu, A. Radu

AU - Jones, E. Yvonne

AU - Szedlacsek, Stefan E.

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Y1 - 2008/3

N2 - Structural analysis of protein tyrosine phosphatases (PTPs) has expanded considerably in the last several years, producing more than 200 structures in this class of enzymes (from 35 different proteins and their complexes with ligands). The small-medium size of the catalytic domain of ∼280 residues plus a very compact fold makes it amenable to cloning and overexpression in bacterial systems thus facilitating crystallographic analysis. The low molecular weight PTPs being even smaller, ∼150 residues, are also perfect targets for NMR analysis. The availability of different structures and complexes of PTPs with substrates and inhibitors has provided a wealth of information with profound effects in the way we understand their biological functions. Developments in mammalian expression technology recently led to the first crystal structure of a receptor-like PTP extracellular region. Altogether, the PTP structural work significantly advanced our knowledge regarding the architecture, regulation and substrate specificity of these enzymes. In this review, we compile the most prominent structural traits that characterize PTPs and their complexes with ligands. We discuss how the data can be used to design further functional experiments and as a basis for drug design given that many PTPs are now considered strategic therapeutic targets for human diseases such as diabetes and cancer. © 2008 The Authors.

AB - Structural analysis of protein tyrosine phosphatases (PTPs) has expanded considerably in the last several years, producing more than 200 structures in this class of enzymes (from 35 different proteins and their complexes with ligands). The small-medium size of the catalytic domain of ∼280 residues plus a very compact fold makes it amenable to cloning and overexpression in bacterial systems thus facilitating crystallographic analysis. The low molecular weight PTPs being even smaller, ∼150 residues, are also perfect targets for NMR analysis. The availability of different structures and complexes of PTPs with substrates and inhibitors has provided a wealth of information with profound effects in the way we understand their biological functions. Developments in mammalian expression technology recently led to the first crystal structure of a receptor-like PTP extracellular region. Altogether, the PTP structural work significantly advanced our knowledge regarding the architecture, regulation and substrate specificity of these enzymes. In this review, we compile the most prominent structural traits that characterize PTPs and their complexes with ligands. We discuss how the data can be used to design further functional experiments and as a basis for drug design given that many PTPs are now considered strategic therapeutic targets for human diseases such as diabetes and cancer. © 2008 The Authors.

KW - Catalytic mechanism

KW - Cell adhesion

KW - Cell signalling

KW - Drug design

KW - Ligand binding

KW - NMR

KW - Phosphatase inhibitor

KW - Protein structure

KW - Protein tyrosine phosphatase

KW - Structure-function receptor

KW - X-ray crystallography

U2 - 10.1111/j.1742-4658.2008.06251.x

DO - 10.1111/j.1742-4658.2008.06251.x

M3 - Article

SN - 1742-4658

VL - 275

SP - 867

EP - 882

JO - FEBS Journal

JF - FEBS Journal

IS - 5

ER -

Protein tyrosine phosphatases: Structure-function relationships

Abstract

Keywords

UN SDGs

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