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Merck

Targeting G protein-coupled receptor signaling at the G protein level with a selective nanobody inhibitor.

Nature communications (2018-05-20)
Sahil Gulati, Hui Jin, Ikuo Masuho, Tivadar Orban, Yuan Cai, Els Pardon, Kirill A Martemyanov, Philip D Kiser, Phoebe L Stewart, Christopher P Ford, Jan Steyaert, Krzysztof Palczewski
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G protein-coupled receptors (GPCRs) activate heterotrimeric G proteins by mediating a GDP to GTP exchange in the Gฮฑ subunit. This leads to dissociation of the heterotrimer into Gฮฑ-GTP and Gฮฒฮณ dimer. The Gฮฑ-GTP and Gฮฒฮณ dimer each regulate a variety of downstream pathways to control various aspects of human physiology. Dysregulated Gฮฒฮณ-signaling is a central element of various neurological and cancer-related anomalies. However, Gฮฒฮณ also serves as a negative regulator of Gฮฑ that is essential for G protein inactivation, and thus has the potential for numerous side effects when targeted therapeutically. Here we report a llama-derived nanobody (Nb5) that binds tightly to the Gฮฒฮณ dimer. Nb5 responds to all combinations of ฮฒ-subtypes and ฮณ-subtypes and competes with other Gฮฒฮณ-regulatory proteins for a common binding site on the Gฮฒฮณ dimer. Despite its inhibitory effect on Gฮฒฮณ-mediated signaling, Nb5 has no effect on Gฮฑq-mediated and Gฮฑs-mediated signaling events in living cells.

MATERIALS
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Millipore
ANTI-FLAGยฎ antibody produced in rabbit, affinity isolated antibody, buffered aqueous solution
Sigma-Aldrich
Anti-Glyceraldehyde-3-Phosphate Dehydrogenase Antibody, clone 6C5, clone 6C5, Chemiconยฎ, from mouse