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Dive into the research topics where Louis Leong is active.

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Featured researches published by Louis Leong.


Nature | 2017

Structural insight into allosteric modulation of protease-activated receptor 2

Robert K. Y. Cheng; Cédric Fiez-Vandal; Oliver Schlenker; Karl Edman; Birte Aggeler; Dean G. Brown; Giles Albert Brown; Robert M. Cooke; Christoph E. Dumelin; Andrew S. Doré; Stefan Geschwindner; Christoph Grebner; Nils-Olov Hermansson; Ali Jazayeri; Patrik Johansson; Louis Leong; Rudi Prihandoko; Mathieu Rappas; Holly H. Soutter; Arjan Snijder; Linda Sundström; Benjamin G. Tehan; Peter Thornton; Dawn M. Troast; Giselle R. Wiggin; Andrei Zhukov; Fiona H. Marshall; Niek Dekker

Protease-activated receptors (PARs) are a family of G-protein-coupled receptors (GPCRs) that are irreversibly activated by proteolytic cleavage of the N terminus, which unmasks a tethered peptide ligand that binds and activates the transmembrane receptor domain, eliciting a cellular cascade in response to inflammatory signals and other stimuli. PARs are implicated in a wide range of diseases, such as cancer and inflammation. PARs have been the subject of major pharmaceutical research efforts but the discovery of small-molecule antagonists that effectively bind them has proved challenging. The only marketed drug targeting a PAR is vorapaxar, a selective antagonist of PAR1 used to prevent thrombosis. The structure of PAR1 in complex with vorapaxar has been reported previously. Despite sequence homology across the PAR isoforms, discovery of PAR2 antagonists has been less successful, although GB88 has been described as a weak antagonist. Here we report crystal structures of PAR2 in complex with two distinct antagonists and a blocking antibody. The antagonist AZ8838 binds in a fully occluded pocket near the extracellular surface. Functional and binding studies reveal that AZ8838 exhibits slow binding kinetics, which is an attractive feature for a PAR2 antagonist competing against a tethered ligand. Antagonist AZ3451 binds to a remote allosteric site outside the helical bundle. We propose that antagonist binding prevents structural rearrangements required for receptor activation and signalling. We also show that a blocking antibody antigen-binding fragment binds to the extracellular surface of PAR2, preventing access of the tethered ligand to the peptide-binding site. These structures provide a basis for the development of selective PAR2 antagonists for a range of therapeutic uses.


Archive | 2001

METHODS AND COMPOSITIONS FOR SYNTHESIS OF NUCLEIC ACID MOLECULES USING MULTIPLE RECOGNITION SITES

Jonathan D. Chesnut; John Carrino; Louis Leong; Knut R. Madden; Martin A. Gleeson; James Fan; Michael A. Brasch; David Cheo; James L. Hartley; Devon R. N. Byrd; Gary F. Temple


Archive | 2004

METHODS AND COMPOSITIONS FOR SEAMLESS CLONING OF NUCLEIC ACID MOLECULES

Jonathan D. Chesnut; Miroslav Dudas; Adam N. Harris; Louis Leong; Knut R. Madden


Archive | 2004

Nucleic acid molecules containing recombination sites and methods of using the same

Jonathan D. Chesnut; Louis Leong


Archive | 2009

CONTROL OF CHEMICAL MODIFICATION

John Matthew Mauro; Thomas Harry Steinberg; Lawrence Greenfield; Louis Leong


Archive | 2009

Stable compositions comprising chromogenic compounds and methods of use

Lawrence Greenfield; Shawn Starkenburg; Matthew Shallice; Julie Nyhus; Louis Leong


Journal of Immunology | 2010

Recombinant Rabbit Monoclonal Antibodies to Study Apoptosis and Apoptotic Pathways

Margaret Lubkin; Matthew Shallice; Julie Nyhus; Louis Leong; Birte Aggeler


Archive | 2009

Compositions stables comprenant des composés chromogènes, et procédés d'utilisation

Lawrence Greenfield; Shawn Starkenburg; Matthew Shallice; Julie Nyhus; Louis Leong


Archive | 2004

Procedes et compositions permettant de detecter une activite de promoteur et d'exprimer des proteines de fusion

Peter J. Welch; Jonathan D. Chesnut; Robert P. Bennett; Kenneth Frimpong; Louis Leong; James Fan; Harry Yim; Laura Vozza-Brown


Archive | 2004

Verfahren und Zusammensetzungen zum nahtlosen Klonieren von Nukleinsäuremolekülen

Jonathan D. Chesnut; Knut R. Madden; Miroslav Dudas; Louis Leong; Adam N. Harris

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David Cheo

University of Texas Southwestern Medical Center

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James L. Hartley

Science Applications International Corporation

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