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Aliphatic Azides as Selective Cysteine Labeling Reagents for Integral Membrane Proteins.

J Med Chem. 2018; 
Szymanski D, Papanastasiou M, Pandarinathan L, Zvonok N, Janero DR, Pavlopoulos S, Vouros P, Makriyannis A.
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Peptide Synthesis The model peptide (P2) corresponding to TM6 of the hCB2 receptor (DVRLAKTLGLVLAVLLICWFPVLALMAHS) was synthesized by Genscript (>95% purity). Get A Quote

摘要

Upon ultraviolet activation, cannabinergic aliphatic azido (N3) ligands covalently label cannabinoid receptors, prominent G-protein-coupled receptor (GPCR) drug targets. We report here the mechanism of covalent attachment to selected substrates of the high-affinity CBR inverse agonist AM1335 and its deuterated analog AM1335(d10), arylpyrazole compounds with an azide moiety at their n-pentyl side chain. To model the receptor interaction, we utilized the human cannabinoid 2 receptor (hCB2R) transmembrane helix 6 (TMH6) peptide and an N-acyl-protected cysteine (NAC). The photochemical reaction products of model substrates with AM1335 and AM1335(d10) were analyzed with tandem electrospray ionization mass spectromet... More

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