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心脏保护剂ICRF - 187[(+)-1,2 - 双(3,5 - 二氧代哌嗪基 - 1 - 基)丙烷];其水解产物(ICRF - 198);以及其他螯合剂与阿霉素的铁(III)和铜(II)配合物的相互作用。

The interaction of the cardioprotective agent ICRF-187 [+)-1,2-bis(3,5-dioxopiperazinyl-1-yL)propane); its hydrolysis product (ICRF-198); and other chelating agents with the Fe(III) and Cu(II) complexes of adriamycin.

作者信息

Hasinoff B B

机构信息

Department of Chemistry, Memorial University of Newfoundland, St. John's, Canada.

出版信息

Agents Actions. 1989 Mar;26(3-4):378-85. doi: 10.1007/BF01967305.

Abstract

Membrane-permeable ICRF-187 [+]-1,2-bis(3,5-dioxopiperazinyl-1-yl)propane) has shown promise as a cardioprotective agent against adriamycin-induced cardiotoxicity. ICRF-187 may act through its rings-opened hydrolysis product (ICRF-198), which has an EDTA-type structure and, likewise, strongly binds metal ions. The reactions of these compounds with Fe3+-adriamycin and Cu2+-adriamycin complexes were examined. ICRF-198 quickly and completely removed both Fe3+ and Cu2+ from their complexes with adriamycin. ICRF-187 also reacted directly, but more slowly, with Fe3+-adriamycin to remove Fe3+ from the complex. This reaction was first order in ICRF-187 and Fe3+-adriamycin and yielded a second order rate constant of 123 M-1 min-1. Metal ion-complex promoted hydrolysis may thus contribute to the in vivo hydrolysis of ICRF-187 to its metal ion-chelating active rings-opened form. Both ICRF-187 and ICRF-198 were very effective in preventing the Fe3+-adriamycin induced inactivation of the cytochrome c oxidase activity of submitochondrial particles. A number of other chelating agents (desferal; penicillamine; DTPA; EDTA; TPEN; bathophenanthroline sulfonic acid; 2,2'-bipyridine; 1.10-phenanthroline, glutathione and 2-mercaptoethanol) were also examined for their ability to remove Fe3+ and Cu2+ from their complexes with adriamycin.

摘要

膜通透性ICRF - 187 [+]-1,2 - 双(3,5 - 二氧代哌嗪基 - 1 - 基)丙烷)已显示出作为一种抗阿霉素诱导的心脏毒性的心脏保护剂的潜力。ICRF - 187可能通过其开环水解产物(ICRF - 198)起作用,该产物具有EDTA型结构,同样能强烈结合金属离子。研究了这些化合物与Fe3 + - 阿霉素和Cu2 + - 阿霉素络合物的反应。ICRF - 198能迅速且完全地从其与阿霉素的络合物中去除Fe3 +和Cu2 +。ICRF - 187也直接与Fe3 + - 阿霉素反应,但速度较慢,从络合物中去除Fe3 +。该反应对ICRF - 187和Fe3 + - 阿霉素为一级反应,二级反应速率常数为123 M-1 min-1。因此,金属离子 - 络合物促进的水解可能有助于ICRF - 187在体内水解为其金属离子螯合的开环形式。ICRF - 187和ICRF - 198在防止Fe3 + - 阿霉素诱导的亚线粒体颗粒细胞色素c氧化酶活性失活方面都非常有效。还研究了许多其他螯合剂(去铁胺;青霉胺;二乙三胺五乙酸;乙二胺四乙酸;三(2 - 吡啶甲基)胺;4,7 - 二苯基 - 1,10 - 菲啰啉磺酸;2,2'-联吡啶;1,10 - 菲啰啉、谷胱甘肽和2 - 巯基乙醇)从其与阿霉素的络合物中去除Fe3 +和Cu2 +的能力。

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