Selectivity of cyclic [D-Nal(7)] and [D-Phe(7)] substituted MSH analogues for the melanocortin receptor subtypes

被引:82
作者
Schioth, HB
Muceniece, R
Mutulis, F
Prusis, P
Lindeberg, G
Sharma, SD
Hruby, VJ
Wikberg, JES
机构
[1] UNIV UPPSALA,DEPT MED & PHYSIOL CHEM,UPPSALA,SWEDEN
[2] INST ORGAN SYNTH,PHARMACOL LAB,RIGA,LATVIA
[3] INST ORGAN SYNTH,DEPT MED CHEM,RIGA,LATVIA
[4] UNIV ARIZONA,DEPT CHEM,TUCSON,AZ 85721
关键词
melanocortin receptor subtypes; MSH; MTII; SHU9119; HS9510; ligand binding;
D O I
10.1016/S0196-9781(97)00079-X
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The binding of the 2 cyclic lactam MSH (4-10) analogues (MTII, 5HU9119), and 5 cyclic [Cys(4), Cys(10)]alpha-MSH analogues were tested on cells transiently expressing the human MC1, MC3, MC4 and MC5 receptors. The results indicate a differential importance of the C-terminal (Lys-Pro-Val) and N-terminal (Ser-Tyr-Ser) of cyclic [Cys(4), Cys(10)]alpha-MSH analogues in binding to the MC receptor subtypes. Substitution of D-Phe(7) by D-Nal(2')(7) in both the cyclic lactam MSH (4-10) and the cyclic disulphide MSH (4-10) analogues resulted in a shift in favour of selectivity for the MC4 receptor; the disulphide analogue, [Cys(4), D-Nal(2')(7) Cys(10)]alpha-MSH (4-10) (HS9510), showing the highest selectivity for the MC4 receptor among all the substances tested. However, the cyclic lactams displayed an over all higher affinity for the MC receptors, than any of the cyclic disulphide MSH (4-10) analogues. (C) 1997 Elsevier Science Inc.
引用
收藏
页码:1009 / 1013
页数:5
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