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声化学促进烷基钴胺素(III)生物共轭物的间接碳-钴键断裂。

Sonolysis promotes indirect Co-C bond cleavage of alkylcob(III)alamin bioconjugates.

作者信息

Howard W A, Bayomi A, Natarajan E, Aziza M A, el-Ahmady O, Grissom C B, West F G

机构信息

Department of Chemistry, University of Utah, Salt Lake City 84112, USA.

出版信息

Bioconjug Chem. 1997 Jul-Aug;8(4):498-502. doi: 10.1021/bc970077l.

Abstract

Sonolysis of aqueous solutions produces H. and HO. that lead to Co-C bond cleavage in methylcob-(III)alamin (CH3-CblIII) and 2-[4-[4'-[bis(2-chloroethyl)amino]phenyl]butyroxy]ethylcob (III)alamin (Chl-HE-CblIII). Under anaerobic conditions, H. reduces CH3-CblIII to the unstable 19 e-CH3-CblII that dissociates to the alkane and CblII. Under aerobic conditions, O2 scavenges H. and Co-C bond cleavage occurs via a HO.-mediated process along with modification of the corrin ring by HO.. When H. and HO. are scavenged, there is no evidence of Co-C bond cleavage. This suggests no direct sonolysis of the Co-C bond occurs, in spite of the fact that the Co-C bond is 80 kcal/mol weaker than the H-OH bond. A bioconjugate of cob(III)alamin and the alkylating agent chlorambucil has been synthesized to give 2-[4-[4'-[bis(2-chloroethyl)amino]phenyl]butyroxy]ethylcob(I II)alamin. The chlorambucil-cobalamin complex also undergoes Co-C bond cleavage in a manner similar to that of methylcob-(III)alamin. Sonorelease of an active alkylating agent from the bioconjugate may provide a new method for the selective release of anticancer drugs and thus potentially reduce systemic toxicity.

摘要

水溶液的声解作用会产生氢原子(H.)和羟基自由基(HO.),它们会导致甲基钴胺素(III)(CH3 - CblIII)和2 - [4 - [4'-[双(2 - 氯乙基)氨基]苯基]丁酰氧基]乙基钴胺素(III)(Chl - HE - CblIII)中的钴 - 碳键断裂。在厌氧条件下,氢原子将CH3 - CblIII还原为不稳定的19电子 - CH3 - CblII,后者会分解为烷烃和CblII。在有氧条件下,O2会清除氢原子,钴 - 碳键的断裂通过羟基自由基介导的过程发生,同时羟基自由基会对卟啉环进行修饰。当氢原子和羟基自由基被清除时,没有证据表明钴 - 碳键会断裂。这表明尽管钴 - 碳键比氢 - 氧键弱80千卡/摩尔,但钴 - 碳键不会直接发生声解。已经合成了钴胺素(III)与烷基化剂苯丁酸氮芥的生物共轭物,得到2 - [4 - [4'-[双(2 - 氯乙基)氨基]苯基]丁酰氧基]乙基钴胺素(I II)。苯丁酸氮芥 - 钴胺素复合物也以类似于甲基钴胺素(III)的方式发生钴 - 碳键断裂。从生物共轭物中声释放活性烷基化剂可能为抗癌药物的选择性释放提供一种新方法,从而有可能降低全身毒性。

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