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Dive into the research topics where James E. Pease is active.

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Featured researches published by James E. Pease.


Molecular Immunology | 1994

Site directed mutagenesis of the complement C5a receptor—Examination of a model for its interaction with the ligand C5a

James E. Pease; Dennis R. Burton; Michael D. Barker

C5a is a 74 amino acid peptide cleaved from the fifth component of the complement system after activation of either the alternative or classical pathways. It is a potent chemoattractant for neutrophils and monocytes binding to identical receptors on the cell surface. Following the cloning of the cDNA encoding for the human complement C5a receptor, revealing it to be a member of the rhodopsin superfamily of G-protein coupled receptors, a model for the interaction of the C5a receptor with its ligand was proposed, the structure for the receptor being modelled on that of the well defined receptor bacteriorhodopsin. In this model two key residues of the receptor, aspartate82 and either glutamate179 or glutamate 180 were proposed to make up part of the binding site for C5a, acting as counter ions for arginine74 and arginine40, respectively of the C5a molecule. Replacement of aspartate82, glutamate179 and glutamate180 of the C5a receptor with asparagine and glutamine, respectively was shown to have little effect on the dissociation constant of the receptor as detected by Scatchard analysis and competitive binding assays. Hence this modus operandi for the interaction of C5a with its receptor can be rejected.


Journal of Immunology | 1997

Molecular cloning of leukotactin-1: a novel human beta-chemokine, a chemoattractant for neutrophils, monocytes, and lymphocytes, and a potent agonist at CC chemokine receptors 1 and 3.

Byung S. Youn; Shang M. Zhang; Eun K. Lee; Doo H. Park; Hal E. Broxmeyer; Philip M. Murphy; Massimo Locati; James E. Pease; Kack K. Kim; Kathleen Antol; Byoung S. Kwon


Journal of Biological Chemistry | 1995

Mutation of Glutamate 199 of the Human C5a Receptor Defines a Binding Site for Ligand Distinct from the Receptor N Terminus

Peter N. Monk; Michael D. Barker; Lynda J. Partridge; James E. Pease


European Journal of Immunology | 1994

Generation of chimeric C5a/formyl peptide receptors: towards the identification of the human C5a receptor binding site

James E. Pease; Dennis R. Burton; Michael D. Barker


Biochemistry | 1999

Receptor activation by human C5a des Arg74 but not intact C5a is dependent on an interaction between Glu199 of the receptor and Lys68 of the ligand.

Torsten Crass; Wilfried Bautsch; Stuart A. Cain; James E. Pease; Peter N. Monk


Iubmb Life | 1994

C5a stimulus-secretion coupling in rat basophilic leukaemia (RBL-2H3) cells transfected with the human C5a receptor is mediated by pertussis and cholera toxin-sensitive G proteins

Peter N. Monk; James E. Pease; Barker


European Journal of Immunology | 1994

Mutation of aspartate 82 of the human C5a receptor abolishes the secretory response to human C5a in transfected rat basophilic leukemia cells

Peter N. Monk; James E. Pease; Gillian Marland; Michael D. Barker


Iubmb Life | 1993

The generation of stable CHO cell lines expressing very high levels of complement C5A receptors and subsequent modulation of binding affinity for C5A.

James E. Pease; Dennis R. Burton; Barker


Immunology Letters | 1997

Chemokine and chemoattractant receptor expression on human endothelial cells

Craig Murdoch; Peter N. Monk; James E. Pease; M.D. Barker; Adam Finn


Immunology Letters | 1997

The functional capacity of chemoattractant receptors expressed on RBL cells correlates with their rates of internalization

M.D. Barker; James E. Pease; Peter N. Monk

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M.D. Barker

University of Sheffield

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Dennis R. Burton

Scripps Research Institute

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Adam Finn

University of Sheffield

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