van Rijt Sabine H, Hebden Andrew J, Amaresekera Thakshila, Deeth Robert J, Clarkson Guy J, Parsons Simon, McGowan Patrick C, Sadler Peter J
Department of Chemistry, University of Warwick, Gibbet Hill Road, Coventry CV4 7AL, UK.
J Med Chem. 2009 Dec 10;52(23):7753-64. doi: 10.1021/jm900731j.
We show that the binding mode adopted by picolinamide derivatives in organometallic Os(II) and Ru(II) half-sandwich complexes can lead to contrasting cancer cell cytotoxicity. N-Phenyl picolinamide derivatives (XY) in Os(II) (1, 3-5, 7, 9) and Ru(II) (2, 6, 8, 10) complexes (eta(6)-arene)(Os/Ru)(XY)Cl, where arene = p-cymene (1-8, 10) or biphenyl (9), can act as N,N- or N,O-donors. Electron-withdrawing substituents on the phenyl ring resulted in N,N-coordination and electron-donating substituents in N,O-coordination. Dynamic interconversion between N,O and N,N configurations can occur in solution and is time- and temperature- (irreversible) as well as pH-dependent (reversible). The neutral N,N-coordinated compounds (1-5 and 9) hydrolyzed rapidly (t(1/2) <or= min), exhibited significant (32-70%) and rapid binding to guanine, but no binding to adenine. The N,N-coordinated compounds 1, 3, 4, and 9 exhibited significant activity against colon, ovarian, and cisplatin-resistant ovarian human cancer cell lines (3 >> 4 > 1 > 9). In contrast, N,O-coordinated complexes 7 and 8 hydrolyzed slowly, did not bind to guanine or adenine, and were nontoxic.
我们表明,吡啶甲酰胺衍生物在有机金属锇(II)和钌(II)半夹心配合物中的结合模式可导致截然不同的癌细胞细胞毒性。锇(II)(1, 3 - 5, 7, 9)和钌(II)(2, 6, 8, 10)配合物(η(6)-芳烃)(Os/Ru)(XY)Cl中的N-苯基吡啶甲酰胺衍生物(XY),其中芳烃 = 对异丙基苯(1 - 8, 10)或联苯(9),可作为N,N-或N,O-供体。苯环上的吸电子取代基导致N,N配位,而供电子取代基导致N,O配位。N,O和N,N构型之间的动态相互转化可在溶液中发生,并且是时间和温度依赖性的(不可逆)以及pH依赖性的(可逆)。中性的N,N配位化合物(1 - 5和9)快速水解(t(1/2)≤分钟),对鸟嘌呤表现出显著(32 - 70%)且快速的结合,但对腺嘌呤无结合。N,N配位化合物1、3、4和9对结肠、卵巢和顺铂耐药的卵巢人癌细胞系表现出显著活性(3 >> 4 > 1 > 9)。相比之下,N,O配位的配合物7和8水解缓慢,不与鸟嘌呤或腺嘌呤结合,且无毒。
