首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Epoxidation of (+/-)-78-dihydroxy-78-dihydrobenzoapyrene during (bi)sulfite autoxidation: activation of a procarcinogen by a cocarcinogen.
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Epoxidation of (+/-)-78-dihydroxy-78-dihydrobenzoapyrene during (bi)sulfite autoxidation: activation of a procarcinogen by a cocarcinogen.

机译:亚硫酸氢盐自氧化过程中(+/-)-78-二羟基-78-二氢苯并a的环氧化:致癌物激活致癌物。

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摘要

The (bi)sulfite ion undergoes extensive autoxidation in neutral aqueous media with the formation of sulfur trioxide radical anion that is detected by ESR. The radical anion subsequently reacts with molecular oxygen to form a peroxyl radical. We find that when (+/-)-trans-7,8-dihydroxy-7,8-dihydrobenzo[a]pyrene (BP-7,8-diol) is included in this autoxidation system, BP-7,8-diol is converted to diolepoxides, ultimate carcinogenic derivatives of benzo[a]pyrene. This epoxidation occurs with a stereoselectivity consistent with either a peroxyl radical or a peracid as the epoxidizing agent. The epoxidation is dependent on the concentration of both (bi)sulfite and oxygen. In the presence of 10 microM butylated hydroxyanisole, which abolishes (bi)sulfite autoxidation, no (bi)sulfite-dependent epoxidation occurs. These results are discussed in regard to the mechanism of (bi)sulfite autoxidation, and in relationship to the cocarcinogenicity of sulfur dioxide [anhydrous (bi)sulfite] for benzo[a]pyrene-induced pulmonary neoplasia.
机译:亚硫酸根离子在中性水性介质中经历广泛的自氧化反应,形成三氧化硫自由基阴离子,该阴离子可通过ESR检测到。自由基阴离子随后与分子氧反应形成过氧自由基。我们发现,当(+/-)-反式-7,8-二羟基-7,8-二氢苯并[a] py(BP-7,8-二醇)被包括在此自氧化系统中时,BP-7,8-二醇被转化为二醇环氧化合物,苯并[a]]的最终致癌衍生物。该环氧化发生的立体选择性与过氧自由基或过酸作为环氧化剂一致。环氧化取决于(亚)亚硫酸氢盐和氧气的浓度。在存在10 microM丁基化羟基茴香醚的情况下,该产物消除了(Bi)亚硫酸盐的自氧化作用,没有发生(Bi)亚硫酸盐依赖性的环氧化反应。讨论了有关(亚硫酸)亚硫酸盐自氧化的机理,以及有关二氧化硫[无水(亚硫酸)亚硫酸盐)对苯并[a] py诱发的肺肿瘤的致癌性的结果。

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