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- W1965507811 abstract "Kisspeptins (KPs) play important roles in the regulation of physiological and pathological states through activation of the cognate receptor GPR54. Our previous studies to downsize KP agonists to the essential GPR54 pharmacophore identified peptides 1−3 as low molecular weight GPR54 agonists. In this study, the effect of N-terminal acyl groups on the activity of a series of analogues (R-Phe-Gly-Leu-Arg-Trp-NH2) was investigated in order to develop novel potent GPR54 agonists. Among the compounds developed, the most potent agonistic activity for GPR54 was observed for N-terminal 4-fluorobenzoyl analogue 29. Using quantitative structure−activity relationship studies, it was demonstrated that the inductively negative and small substituents were preferred at the 4-position of N-terminal benzoyl groups." @default.
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- W1965507811 date "2007-06-19" @default.
- W1965507811 modified "2023-09-28" @default.
- W1965507811 title "SAR and QSAR Studies on the N-Terminally Acylated Pentapeptide Agonists for GPR54" @default.
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- W1965507811 doi "https://doi.org/10.1021/jm070064l" @default.
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