Sphingosine-1-Phosphate and Its Receptors: Structure, Signaling, and Influence

Author:

Rosen Hugh12,Stevens Raymond C.3,Hanson Michael4,Roberts Edward5,Oldstone Michael B.A.6

Affiliation:

1. Department of Chemical Physiology and Immunology,

2. The Scripps Research Institute Molecular Screening Center,

3. Department of Molecular Biology,

4. Receptos Inc., San Diego, California 92121;

5. Department of Chemistry, and

6. Department of Immunology and Microbial Sciences, The Scripps Research Institute, La Jolla, California 92037;, , ,

Abstract

The sphingosine-1-phosphate (S1P) receptor signaling system has biological and medical importance and is the first lipid G protein–coupled receptor (GPCR) structure to be solved to 2.8-Å resolution. S1P binds to five high-affinity GPCRs generating multiple downstream signals that play essential roles in vascular development and endothelial integrity, control of cardiac rhythm, and routine oral treatment of multiple sclerosis. Genetics, chemistry, and now structural biology have advanced this integrated biochemical system. The S1P receptors have a novel N-terminal fold that occludes access to the binding pocket from the extracellular environment as well as orthosteric and bitopic ligands with very different physicochemical properties. S1P receptors and metabolizing enzymes have been deleted, inducibly deleted, and knocked in as tagged or altered receptors in mice. An array of genetic models allows analysis of integrated receptor function in vivo. We can now directly understand causal relationships among protein expression, signal, and control points in physiology and pathology.

Publisher

Annual Reviews

Subject

Biochemistry

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