Potent P2X 7 Receptor Antagonists: Tyrosyl Derivatives Synthesized Using a Sequential Parallel Synthetic Approach
Novel analogs of 1-( , -bis[5-isoquinolinesulfonyl]-N-methyl-L-tyrosyl)-4-phenylpiperazine (KN-62,1) were synthesized and found to be potent antagonists in a functional assay, inhibition of ATP-induced K efflux in HEK293 cells expressing recombinant human P2X receptors. Antagonism of murine P2X rece...
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Veröffentlicht in: | Drug development research 2001-10, Vol.54 (2), p.75-87 |
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Hauptverfasser: | , , , |
Format: | Artikel |
Sprache: | eng |
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Zusammenfassung: | Novel analogs of 1-(
,
-bis[5-isoquinolinesulfonyl]-N-methyl-L-tyrosyl)-4-phenylpiperazine (KN-62,1) were synthesized and found to be potent antagonists in a functional assay, inhibition of ATP-induced K
efflux in HEK293 cells expressing recombinant human P2X
receptors. Antagonism of murine P2X
receptors was also observed. The analogs consisted of L-tyrosine derivatives, of the general structure R
-Tyr(OR
)-piperazinyl-R
, in which three positions were systematically varied in structure through facile acylation reactions. Each of the three positions was optimized in sequence through parallel synthesis alternating with biological evaluation, leading to the identification and optimization of potent P2X
antagonists. The optimal groups at R
were found to be large hydrophobic groups, linked to the α-amino position through carbamate, amide, or sulfonamide groups. The benzyloxycarbonyl (Cbz) group was preferred over most sulfonamides and other acyl groups examined, except for quinoline sulfonyl. At R
, an arylsulfonate ester was preferred, and the order of potency was p-tolyl, p-methoxyphenyl, phenyl > α-naphthyl, β-naphthyl. A benzoyl ester was of intermediate potency. Aliphatic esters and carbonate derivatives at the tyrosyl phenol were inactive, while a tyrosyl O-benzyl ether was relatively potent. The most potent P2X
receptor antagonists identified in this study contained Cbz at the R
position, an aryl sulfonate at the R
position, and various acyl groups at the R
position. At R
,
-butyloxycarbonyl- and benzoyl groups were preferred. The opening of the piperazinyl ring to an ethylene diamine moiety abolished antagonism. In concentration-response studies, a di-isoquinolinyl, Boc derivative,
(MRS2306), displayed an IC
value of 40 nM as an antagonist of P2X
receptor-mediated ion flux and was more potent than the reference compound
. N
-Cbz, Boc-piperazinyl derivatives,
(MRS2317),
(MRS2326), and
(MRS2409) were less potent than
, with IC
values of 200-300 nM. |
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ISSN: | 0272-4391 1098-2299 |
DOI: | 10.1002/ddr.1207 |