Characterization of Protease-activated Receptor-2 Immunoreactivity in Normal Human Tissues

Author:

R. D'Andrea Michael1,Derian Claudia K.1,Leturcq Didier2,Baker Sherry M.2,Brunmark Anders2,Ling Ping2,Darrow Andrew L.1,Santulli Rosemary J.1,Brass Lawrence F.3,Andrade–Gordon Patricia1

Affiliation:

1. Drug Discovery Research, The R.W. Johnson Pharmaceutical Research Institute, Spring House, Pennsylvania

2. La Jolla, California

3. Department of Medicine and Pathology, University of Pennsylvania, Philadelphia, Pennsylvania

Abstract

PAR-2 is a second member of a novel family of G-protein-coupled receptors characterized by a proteolytic cleavage of the amino terminus, thus exposing a tethered peptide ligand that autoactivates the receptor. The physiological and/or pathological role(s) of PAR-2 are still unknown. This study provides tissue-specific cellular localization of PAR-2 in normal human tissues by immunohistochemical techniques. A polyclonal antibody, PAR-2C, was raised against a peptide corresponding to the amino terminal sequence SLIGKVDGTSHVTGKGV of human PAR-2. Significant PAR-2 immunoreactivity was detected in smooth muscle of vascular and nonvascular origin and stromal cells from a variety of tissues. PAR-2 was also present in endothelial and epithelial cells independent of tissue type. Strong immunolabeling was observed throughout the gastrointestinal tract, indicating a possible function for PAR-2 in this system. In the CNS, PAR-2 was localized to many astrocytes and neurons, suggesting involvement of PAR-2 in neuronal function. A role for PAR-2 in the skin was further supported by its immunolocalization in the epidermis. PAR-2C antibody exemplifies an important tool to address the physiological role(s) of PAR-2.

Publisher

SAGE Publications

Subject

Histology,Anatomy

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