1. Academic Validation
  2. The orphan GPCR GPR87 was deorphanized and shown to be a lysophosphatidic acid receptor

The orphan GPCR GPR87 was deorphanized and shown to be a lysophosphatidic acid receptor

  • Biochem Biophys Res Commun. 2007 Nov 23;363(3):861-6. doi: 10.1016/j.bbrc.2007.09.063.
Ken-ichi Tabata 1 Kiyoshi Baba Akira Shiraishi Masahiro Ito Norihisa Fujita
Affiliations

Affiliation

  • 1 Laboratory of Pharmcoinformatics, Department of Bioscience and Bioinformatics, Ritsumeikan University, Kusatsu, Shiga 525-8577, Japan.
Abstract

In CHO cells stably expressing the GPR87 fused with a G16alpha protein, lysophosphatidic acid (LPA) evoked an intracellular CA(2+) increase in a high affinity manner. The CA(2+) increase was reversibly blocked by the LPA receptor antagonists and inhibited by pretreatment of the cells with GPR87-specific siRNAs. GPR87 was shown to be closer to the P2Y and P2Y-related receptors than LPA receptors by ClustalW analyses. However, none of nucleotides and their derivatives activated GPR87. The human gpr87 is located on the chromosome 3q25 in a cluster containing p2y12,13,14. RT-PCR analysis showed that the mouse GPR87 was expressed in placenta, ovary, testis, prostate, brain, and skeletal muscle. The 3D model of GPR87-LPA complex indicated that the ligand interacted with R115 and K296 of GPR87, which are well conserved in the P2Y receptors. These results suggest that the GPR87 is a LPA receptor which evolved from a common ancestor of P2Y receptors.

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