Balaji V N, Ramnarayan K, Chan M F, Rao S N
ImmunoPharmaceutics Inc., San Diego, CA, USA.
Pept Res. 1995 May-Jun;8(3):178-86.
Conformationally constrained peptidomimetics are being increasingly used in the development of 3-D pharmacophores of peptide-based drug candidates and to alter their metabolic stability towards achievements of oral bioavailability. Here we present conformational energy calculations on model compounds containing 1-aminocyclobutane carboxylic acid (ACBC) and its derivatives using molecular mechanics methods. The low-energy models adopt conformations characteristic of a variety of regular structures such as the alpha-helix, 3(10)-helix, gamma-turn and polyproline-II-type three- and fourfold helices. The energetically most favored models adopt the gamma-turn (2.2(7) helix) conformation or alpha-/3(10)-helical conformation, both of either handedness, depending on the substituents on the cyclobutane. These results are qualitatively consistent with the crystal structures of peptide analogs containing ACBC and have implications for the design of peptidomimetics.
构象受限的肽模拟物越来越多地用于基于肽的候选药物的三维药效团开发,并改变其代谢稳定性以实现口服生物利用度。在此,我们使用分子力学方法对含有1-氨基环丁烷羧酸(ACBC)及其衍生物的模型化合物进行构象能量计算。低能量模型采用多种规则结构的特征构象,如α-螺旋、3(10)-螺旋、γ-转角和多聚脯氨酸-II型三螺旋和四螺旋。能量上最有利的模型采用γ-转角(2.2(7)螺旋)构象或α-/3(10)-螺旋构象,二者的手性取决于环丁烷上的取代基。这些结果在定性上与含有ACBC的肽类似物的晶体结构一致,并对肽模拟物的设计具有启示意义。
