Leschke C, Storm R, Breitweg-Lehmann E, Exner T, Nürnberg B, Schunack W
Institut für Pharmazie I, Freie Universität Berlin, Germany.
J Med Chem. 1997 Sep 12;40(19):3130-9. doi: 10.1021/jm9703092.
Synthesis and pharmacological properties of new potent direct activators of heterotrimeric G proteins are described. Compounds were synthesized from protected amino acids with alkylamines using coupling reagents (CDI, DCC, and EDC). Alkyl-substituted amino acid amides and their corresponding di- and triamines were subjected to structure-activity analysis. All compounds activated membrane-bound HL-60 GTPases in a pertussis toxin-sensitive fashion. This suggests a specific effect of compounds on the carboxy terminus of a defined subclass of heterotrimeric G proteins, i.e., members of the G alpha i subfamily. Elongation of the alkyl chain and increasing the number of amino groups enhanced the potency of compounds on HL-60 membrane-bound GTPase. N-(2,5-Diaminopentyl)dodecylamine (21) was selected to study its mode of action employing purified pertussis toxin-sensitive G proteins. It stimulated G alpha subunits by inducing the release of bound GDP. In contrast to receptors G beta gamma complexes were not required for 21-mediated activation of G alpha. Moderate isoform selectivity of its action was observed within a group of highly homologous members of the Gi subfamily with G alpha o1 being activated at lowest concentrations, whereas higher concentrations were necessary for the stimulation of G alpha i1 or transducin. We conclude that these compounds represent important tools for studying G protein-dependent cellular functions.
描述了新型高效异源三聚体G蛋白直接激活剂的合成及其药理特性。使用偶联试剂(CDI、DCC和EDC)由受保护的氨基酸与烷基胺合成化合物。对烷基取代的氨基酸酰胺及其相应的二胺和三胺进行构效分析。所有化合物均以百日咳毒素敏感的方式激活膜结合的HL-60 GTP酶。这表明化合物对特定亚类异源三聚体G蛋白的羧基末端有特异性作用,即Gαi亚家族的成员。烷基链的延长和氨基数量的增加增强了化合物对HL-60膜结合GTP酶的活性。选择N-(2,5-二氨基戊基)十二烷基胺(21),利用纯化的百日咳毒素敏感G蛋白研究其作用方式。它通过诱导结合的GDP释放来刺激Gα亚基。与受体不同,Gβγ复合物对于21介导的Gα激活不是必需的。在Gi亚家族的一组高度同源成员中观察到其作用具有适度的亚型选择性,其中Gαo1在最低浓度下被激活,而刺激Gαi1或转导素则需要更高的浓度。我们得出结论,这些化合物是研究G蛋白依赖性细胞功能的重要工具。
