| Literature DB >> 34613641 |
Adam T Brockett1, Chunlin Deng2, Michael Shuster3, Suvenika Perera2, Delaney DiMaggio2, Ming Cheng2, Steven Murkli2, Volker Briken3, Matthew R Roesch1, Lyle Isaacs2.
Abstract
We report the synthesis of two new acyclic sulfated acyclic CB[n]-type receptors (TriM0 and Me4 TetM0) and investigations of their binding properties toward a panel of drugs of abuse (1-13) by a combination of 1 H NMR spectroscopy and isothermal titration calorimetry. TetM0 is the most potent receptor with Ka ≥106 M-1 toward methamphetamine, fentanyl, MDMA and mephedrone. TetM0 is not cytotoxic toward HepG2 and HEK 293 cells below 100 μM according to MTS metabolic and adenylate kinase release assays and is well tolerated in vivo when dosed at 46 mg kg-1 . TetM0 does not inhibit the hERG ion channel and is not mutagenic based on the Ames fluctuation test. Finally, in vivo efficacy studies show that the hyperlocomotion of mice treated with methamphetamine can be greatly reduced by treatment with TetM0 up to 5 minutes later. TetM0 has potential as a broad spectrum in vivo sequestrant for drugs of abuse.Entities:
Keywords: cucurbituril; hyperlocomotion; methamphetamine; molecular recognition; sequestration agents
Mesh:
Substances:
Year: 2021 PMID: 34613641 PMCID: PMC8665056 DOI: 10.1002/chem.202102919
Source DB: PubMed Journal: Chemistry ISSN: 0947-6539 Impact factor: 5.236