Hanaki Yusuke, Yanagita Ryo C, Sugahara Takahiro, Aida Misako, Tokuda Harukuni, Suzuki Nobutaka, Irie Kazuhiro
a Division of Food Science and Biotechnology , Graduate School of Agriculture, Kyoto University , Kyoto , Japan.
Biosci Biotechnol Biochem. 2015;79(6):888-95. doi: 10.1080/09168451.2014.1002452. Epub 2015 Jan 23.
Aplog-1 is a simplified analog of the tumor-promoting aplysiatoxin with anti-proliferative and cytotoxic activities against several cancer cell lines. Our recent findings have suggested that protein kinase Cδ (PKCδ) could be one of the target proteins of aplog-1. In this study, we synthesized amide-aplog-1 (3), in which the C-1 ester group was replaced with an amide group, to improve chemical stability in vivo. Unfortunately, 3 exhibited seventy-fold weaker binding affinity to the C1B domain of PKCδ than that of aplog-1, and negligible anti-proliferative and cytotoxic activities even at 10(-4) M. A conformational analysis and density functional theory calculations indicated that the stable conformation of 3 differed from that of aplog-1. Since 27-methyl and 27-methoxy derivatives (1, 2) without the ability to bind to PKC isozymes exhibited marked anti-proliferative and cytotoxic activities at 10(-4) M, 3 may be an inactive control to identify the target proteins of aplogs.
Aplog-1是促肿瘤海兔毒素的一种简化类似物,对多种癌细胞系具有抗增殖和细胞毒性活性。我们最近的研究结果表明,蛋白激酶Cδ(PKCδ)可能是aplog-1的靶蛋白之一。在本研究中,我们合成了酰胺-aplog-1(3),其中C-1酯基被酰胺基取代,以提高其体内化学稳定性。不幸的是,3与PKCδ的C1B结构域的结合亲和力比aplog-1弱70倍,即使在10^(-4) M时也几乎没有抗增殖和细胞毒性活性。构象分析和密度泛函理论计算表明,3的稳定构象与aplog-1不同。由于不具有与PKC同工酶结合能力的27-甲基和27-甲氧基衍生物(1, 2)在10^(-4) M时表现出显著的抗增殖和细胞毒性活性,3可能是用于鉴定aplogs靶蛋白的无活性对照。
