Hingerty B, Broyde S
Health and Safety Research Division, Oak Ridge National Laboratory, TN 37830.
J Biomol Struct Dyn. 1983 Dec;1(4):905-12. doi: 10.1080/07391102.1983.10507492.
The (+) anti isomer of benz[a]pyrene diol epoxide (BPDE), 7 beta, 8 alpha-dihydroxy-9 alpha, 10 alpha-epoxy-7,8,9,10-tetrahydrobenz [a] pyrene has been identified as the probable tumorigenic lesion in mammalian systems. It forms a predominant adduct with DNA at N2 of guanine. In order to elucidate its conformation in atomic resolution detail, minimized conformational potential energy calculations were performed for the adduct with dCpdG. A global conformation search involving about 1000 trials was made. The lowest energy conformation had stacking between the hydrocarbon and the adjacent cytidine, in agreement with CD studies on modified GpU and UpG. This conformer differed from the B form most notably in the guanine glycosidic torsion, which is high anti. The next lowest energy form had torsion angles like the B form, with guanine-cytidine stacking. These two conformers differ in energy by only 2.1 kcal./mole, suggesting that their relative stability could easily be reversed in larger polymers, or under specific environmental conditions. Other conformations, with base-hydrocarbon or base-base stacking are also found, at somewhat higher energies. The Z form is at 7.8 kcal./mole. Thus, this adduct stabilizes the B form, in contrast with the N2 linked AAF adduct, which stabilizes the Z conformation.
苯并[a]芘二醇环氧化物(BPDE)的(+)反式异构体,即7β,8α-二羟基-9α,10α-环氧-7,8,9,10-四氢苯并[a]芘,已被确定为哺乳动物系统中可能的致瘤性病变。它在鸟嘌呤的N2处与DNA形成主要加合物。为了在原子分辨率细节上阐明其构象,对与dCpdG形成的加合物进行了最小化构象势能计算。进行了大约1000次试验的全局构象搜索。能量最低的构象是烃与相邻胞嘧啶之间存在堆积,这与对修饰的GpU和UpG的圆二色性研究结果一致。该构象异构体与B型最显著的不同在于鸟嘌呤糖苷扭转角,其为高反式。能量次低的构象具有类似B型的扭转角,存在鸟嘌呤-胞嘧啶堆积。这两种构象异构体的能量仅相差2.1千卡/摩尔,这表明在更大的聚合物中或特定环境条件下,它们的相对稳定性可能很容易反转。还发现了其他具有碱基-烃或碱基-碱基堆积的构象,能量略高。Z型构象的能量为7.8千卡/摩尔。因此,与稳定Z构象的N2连接的AAF加合物相反,这种加合物稳定了B型构象。
