Substituted 7‑Amino-5-thio-thiazolo[4,5‑d]pyrimidines as Potent and Selective Antagonists of the Fractalkine Receptor (CX3CR1)

Substituted 7‑Amino-5-thio-thiazolo[4,5‑d]pyrimidines as Potent and Selective Antagonists of the Fractalkine Receptor (CX3CR1)

We have developed two parallel series, A and B, of CX3CR1 antagonists for the treatment of multiple sclerosis. By modifying the substituents on the 7-amino-5-thio-thiazolo[4,5-d]pyrimidine core structure, we were able to achieve compounds with high selectivity for CX3CR1 over the closely related CXC...

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Veröffentlicht in:Journal of medicinal chemistry 2013-04, Vol.56 (8), p.3177-3190
Hauptverfasser: Karlström, Sofia, Nordvall, Gunnar, Sohn, Daniel, Hettman, Andreas, Turek, Dominika, Åhlin, Kristofer, Kers, Annika, Claesson, Martina, Slivo, Can, Lo-Alfredsson, Yvonne, Petersson, Carl, Bessidskaia, Galina, Svensson, Per H, Rein, Tobias, Jerning, Eva, Malmberg, Åsa, Ahlgen, Charlotte, Ray, Colin, Vares, Lauri, Ivanov, Vladimir, Johansson, Rolf
Format: Artikel
Sprache:eng
Schlagworte:
Amino Alcohols - chemical synthesis
Amino Alcohols - pharmacokinetics
Amino Alcohols - pharmacology
Animals
Caco-2 Cells
CX3C Chemokine Receptor 1
Humans
Multiple Sclerosis - drug therapy
Pyrimidines - chemical synthesis
Pyrimidines - chemistry
Pyrimidines - pharmacokinetics
Pyrimidines - pharmacology
Rats
Receptors, Chemokine - antagonists & inhibitors
Structure-Activity Relationship
Thiazoles - chemical synthesis
Thiazoles - chemistry
Thiazoles - pharmacokinetics
Thiazoles - pharmacology
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Zusammenfassung:We have developed two parallel series, A and B, of CX3CR1 antagonists for the treatment of multiple sclerosis. By modifying the substituents on the 7-amino-5-thio-thiazolo[4,5-d]pyrimidine core structure, we were able to achieve compounds with high selectivity for CX3CR1 over the closely related CXCR2 receptor. The structure–activity relationships showed that a leucinol moiety attached to the core-structure in the 7-position together with α-methyl branched benzyl derivatives in the 5-position displayed promising affinity, and selectivity as well as physicochemical properties, as exemplified by compounds 18a and 24h. We show the preparation of the first potent and selective orally available CX3CR1 antagonists.
ISSN:0022-2623
1520-4804
DOI:10.1021/jm3012273