Cheatham S, Kook A, Hurley L H, Barkley M D, Remers W
Division of Medicinal Chemistry, College of Pharmacy, University of Texas, Austin 78712.
J Med Chem. 1988 Mar;31(3):583-90. doi: 10.1021/jm00398a016.
Tomaymycin is a member of the pyrrolo[1,4]benzodiazepine antitumor-antibiotic group that binds covalently to the exocyclic 2-amino group of guanine in DNA. Previous correlation of fluorescence and NMR data suggested that the 11R,11aS and the 11S,11aS diastereomers of tomaymycin could bind to DNA in two orientations relative to the covalently modified guanine (Barkley, M. D.; Cheatham, S.; Thurston, D. E.; Hurley, L. H. Biochemistry 1986, 25, 3021-3031). We now report on fluorescence, one- and two-dimensional proton NMR, and molecular modeling studies of the tomaymycin-d(ATGCAT)2 adduct, which corroborate these earlier observations. Fluorescence measurements show that there are two species of tomaymycin bound to d(ATGCAT)2, which are tentatively identified as the 11R,11aS and 11S,11aS diastereomers. Two distinct sets of signals for the tomaymycin molecule are present in the proton NMR spectrum of the tomaymycin-d(ATGCAT)2 duplex adduct. Two-dimensional correlation spectroscopy (2D-COSY) studies also show connectivities for four cytosine H5-H6 and eight thymine methyl-H6 protons and thus clearly establish the presence of two distinct species of tomaymycin-d(ATGCAT)2 adducts in solution. A single scalar 11-11a 1H NMR coupling in the 2D-COSY spectrum is indicative of an adduct species that has an S configuration at the C-11 position. Two-dimensional nuclear Overhauser effect (NOESY) spectra of the tomaymycin-d(ATGCAT)2 duplex adduct show that the adducts are relatively nondistortive. In a NOESY experiment, cross-peaks were identified between both the aromatic H9 proton and the ethylidine methyl protons of tomaymycin and two different adenine H2 protons of d(ATGCAT)2. Molecular mechanics calculations with AMBER show that the two species with the thermodynamically most favorable binding energies are the 11R,11aS and 11S,11aS isomers with their aromatic rings to the 5' and 3' sides of the covalently bound guanine, respectively. The NOEs observed between tomaymycin protons and adenine H2 protons are in accord with molecular modeling studies. Taken together, these results strongly suggest that the two forms of tomaymycin bound to d(ATGCAT)2 are the 11S,11aS and 11R,11aS species, oriented with their aromatic rings to the 3' and 5' sides, respectively, of the covalently modified guanines.
托马霉素是吡咯并[1,4]苯并二氮杂卓类抗肿瘤抗生素中的一员,它能与DNA中鸟嘌呤的环外2-氨基共价结合。先前荧光和核磁共振数据的相关性表明,托马霉素的11R,11aS和11S,11aS非对映异构体相对于共价修饰的鸟嘌呤可以两种取向与DNA结合(巴克利,M.D.;切瑟姆,S.;瑟斯顿,D.E.;赫尔利,L.H.《生物化学》,1986年,第25卷,3021 - 3031页)。我们现在报告托马霉素 - d(ATGCAT)₂加合物的荧光、一维和二维质子核磁共振以及分子模拟研究,这些研究证实了早期的这些观察结果。荧光测量表明,有两种托马霉素与d(ATGCAT)₂结合,初步鉴定为11R,11aS和11S,11aS非对映异构体。在托马霉素 - d(ATGCAT)₂双链加合物的质子核磁共振谱中存在托马霉素分子的两组不同信号。二维相关光谱(2D - COSY)研究还显示了四个胞嘧啶H5 - H6和八个胸腺嘧啶甲基 - H6质子的连接性,从而清楚地确定溶液中存在两种不同的托马霉素 - d(ATGCAT)₂加合物。二维COSY谱中的单个标量11 - 11a¹H核磁共振耦合表明加合物在C - 11位置具有S构型。托马霉素 - d(ATGCAT)₂双链加合物的二维核Overhauser效应(NOESY)谱表明加合物相对无扭曲。在一个NOESY实验中,在托马霉素的芳香族H9质子和亚乙基甲基质子与d(ATGCAT)₂的两个不同腺嘌呤H2质子之间鉴定出了交叉峰。使用AMBER进行的分子力学计算表明,具有热力学上最有利结合能的两种物种是11R,11aS和11S,11aS异构体,它们的芳香环分别位于共价结合鸟嘌呤的5'和3'侧。在托马霉素质子与腺嘌呤H2质子之间观察到的核Overhauser效应与分子模拟研究一致。综上所述,这些结果强烈表明与d(ATGCAT)₂结合的两种托马霉素形式是11S,11aS和11R,11aS物种,它们的芳香环分别位于共价修饰鸟嘌呤的3'和5'侧。
