Your search keyword '"Rainish A"' showing total 3 results

1. A bitter anti-inflammatory drug binds at two distinct sites of a human bitter taste GPCR

Author

Lior Peri, Donna Matzov, Dominic R. Huxley, Alon Rainish, Fabrizio Fierro, Liel Sapir, Tara Pfeiffer, Lukas Waterloo, Harald Hübner, Yoav Peleg, Peter Gmeiner, Peter J. McCormick, Dorothee Weikert, Masha Y. Niv, and Moran Shalev-Benami

Subjects

Science

Abstract

Abstract Bitter taste receptors (TAS2Rs), a subfamily of G-protein coupled receptors (GPCRs) expressed orally and extraorally, elicit signaling in response to a large set of tastants. Among 25 functional TAS2Rs encoded in the human genome, TAS2R14 is the most promiscuous, and responds to hundreds of chemically diverse ligands. Here we present the cryo–electron microscopy (cryo-EM) structure of the human TAS2R14 in complex with its signaling partner gustducin, and bound to flufenamic acid (FFA), a clinically approved nonsteroidal anti-inflammatory drug. The structure reveals an unusual binding mode, where two copies of FFA are bound at distinct pockets: one at the canonical receptor site within the trans-membrane bundle, and the other in the intracellular facet, bridging the receptor with gustducin. Together with a pocket-specific BRET-based ligand binding assay, these results illuminate bitter taste signaling and provide tools for a site-targeted compound design.

Published

2024

2. A bitter anti-inflammatory drug binds at two distinct sites of a human bitter taste GPCR.

Author

Peri, Lior, Matzov, Donna, Huxley, Dominic R., Rainish, Alon, Fierro, Fabrizio, Sapir, Liel, Pfeiffer, Tara, Waterloo, Lukas, Hübner, Harald, Peleg, Yoav, Gmeiner, Peter, McCormick, Peter J., Weikert, Dorothee, Niv, Masha Y., and Shalev-Benami, Moran

Abstract

Bitter taste receptors (TAS2Rs), a subfamily of G-protein coupled receptors (GPCRs) expressed orally and extraorally, elicit signaling in response to a large set of tastants. Among 25 functional TAS2Rs encoded in the human genome, TAS2R14 is the most promiscuous, and responds to hundreds of chemically diverse ligands. Here we present the cryo–electron microscopy (cryo-EM) structure of the human TAS2R14 in complex with its signaling partner gustducin, and bound to flufenamic acid (FFA), a clinically approved nonsteroidal anti-inflammatory drug. The structure reveals an unusual binding mode, where two copies of FFA are bound at distinct pockets: one at the canonical receptor site within the trans-membrane bundle, and the other in the intracellular facet, bridging the receptor with gustducin. Together with a pocket-specific BRET-based ligand binding assay, these results illuminate bitter taste signaling and provide tools for a site-targeted compound design. Bitter taste receptors (TAS2Rs) are a subfamily of G-protein coupled receptors (GPCRs). Here, the authors report a cryo-EM structure of the human TAS2R14 in complex with its signaling partner gustducin, and bound to an anti-inflammatory drug flufenamic acid (FFA). [ABSTRACT FROM AUTHOR]

Published

2024

3. Intracellular binding pocket revealed in the human bitter taste receptor TAS2R14

Author

Peri, Lior, primary, Matzov, Donna, additional, Huxley, Dominic R., additional, Rainish, Alon, additional, Fierro, Fabrizio, additional, Sapir, Liel, additional, Pfeiffer, Tara, additional, Waterloo, Lukas, additional, Hübner, Harald, additional, Weikert, Dorothee, additional, Peleg, Yoav, additional, Gmeiner, Peter, additional, McCormick, Peter J., additional, Niv, Masha Y., additional, and Shalev-Benami, Moran, additional

Published

2024