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The effect of substance P and its common in vivo-formed metabolites on MRGPRX2 and human mast cell activation

Pharmacol Res Perspect. 2022-08; 
Lin Hsin, Nithya A Fernandopulle, Jie Ding, Chris Lumb, Nicholas Veldhuis, John A Karas, Susan E Northfield, Graham A Mackay
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Mammalian Expression … explicitly investigated, based on the retention of the polycationic N terminus in SP(1–9) and SP(1… co-transfection with a human MRGPRX2 construct (Genscript) and human Gα15 (cDNA … Get A Quote

摘要

The tachykinin neuropeptide substance P (SP) is the canonical agonist peptide for the neurokinin 1 receptor (NK R). More recently, it has also been shown to activate the Mas-related G protein-coupled receptor X2 (MRGPRX2) receptor on mast cells (MCs), triggering degranulation and release of inflammatory mediators. SP undergoes rapid C-terminal truncation in vivo by a number of proteases to generate the metabolites SP(1-9)-COOH and in particular SP(1-7)-COOH. While the C terminus of SP is critical for NK R activation, studies have shown that the peptide polycationic N terminus is key for MRGPRX2 and mast cell activation. The study thus aimed to determine if the C-terminally truncated metabolites of SP, SP(1-9)-C... More

关键词

MRGPRX2, NK1R, mast cells, neuroinflammation, substance P