Rational design of high affinity tachykinin NK2 receptor antagonists

Artigo Revisado por pares

Rational design of high affinity tachykinin NK2 receptor antagonists

1994; Elsevier BV; Volume: 2; Issue: 2 Linguagem: Inglês

10.1016/s0968-0896(00)82006-4

ISSN

1464-3391

Autores

S. Boyle, Steven Guard, Julie Hodgson, David C. Horwell, William Howson, Joel W. Hughes, A.T. McKnight, K. Martin, Martyn C. Pritchard, Keith J. Watling, G.N. Woodruff,

Tópico(s)

Chemical Synthesis and Analysis

Resumo

The rational discovery of a high affinity NK2 receptor antagonist is described utilizing a general strategy for peptoid design. The contribution to NK2 receptor binding affinity for each amino acid of the hexapeptide 'minimum fragment': Leu-Met-Gln-Trp-Phe-GlyNH2 (8c), was examined by preparing derivatives where each amino acid in turn was replaced with Ala in an 'alanine scan'. The results from this study indicated the primary importance of the Trp and Phe side-chain for binding and led to the observation that Z-Trp-PheNH2 (9a) is a micromolar affinity NK2 receptor dipeptide lead. Further exploration of structure-affinity via conformationally restricted analogues and N- and C-terminus modifications gave a selective, nanomolar affinity NK2 receptor antagonist, (2,3di-CH3OPh)CH2OCO(S)Trp(S)alpha-MePheGlyNH2, PD 147714 (19) with an K(i) = 1.4 nM (hamster urinary bladder membranes and using [125I]-iodohistidyl-NKA (0.1 nM) as the radioligand).

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Rational design of high affinity tachykinin NK2 receptor antagonists