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抗癌剂的光致敏作用。11. 二氨基蒽醌对人白血病细胞的光致敏作用机制:单线态氧和自由基反应。

Photosensitization by anticancer agents. 11. Mechanisms of photosensitization of human leukemic cells by diaminoanthraquinones: singlet oxygen and radical reactions.

作者信息

Reszka K J, Bilski P, Chignell C F, Hartley J A, Khan N, Souhami R L, Mendonca A J, Lown J W

机构信息

Laboratory of Molecular Biophysics, National Institute of Environmental Health Sciences, Research Triangle Park, NC 27709.

出版信息

J Photochem Photobiol B. 1992 Sep 15;15(4):317-35. doi: 10.1016/1011-1344(92)85138-k.

Abstract

The synthesis of several aminoanthraquinone derivatives (AAQs), designed to suppress the dark toxicity and to promote more efficient cancer cell photosensitization for potential use in photodynamic therapy (PDT), is described. The following AAQs were synthesized: 1-NH2-4,5-(MeO)2-AQ (1), 1,5-(NH2)2-4,8-(MeO)2-AQ (2), 1,8-(NH2)2-4,5-(MeO)2-AQ (3), and 1,5-(NHPhMe)2-4,8-(MeO)2-AQ (8). The agents exhibit strong absorption in the region 480-620 nm. Possible mechanisms of photosensitization were studied by measuring 1O2 phosphorescence at 1270 nm, detecting superoxide radicals employing an electron paramagnetic resonance (EPR)-spin trapping technique, and measuring oxygen consumption during the photo-oxidation of a representative biological electron donor, NADH. Strong phosphorescence from 1O2 was observed upon illumination of 2 and 3 in C6H6 (quantum yield of 0.25 and 0.5 respectively), and in EtOH (quantum yield of 0.23 and 0.34). The 1-amino-AQ (1) was the weakest 1O2 sensitizer, with quantum yield of 0.13 in benzene. No phosphorescence was observed in EtOH. A superoxide radical was detected as a spin adduct of 5,5-dimethyl-1-pyrroline-N-oxide (DMPO) in irradiated benzene solutions of 1, 2 or 3 and DMPO. AAQs 2 and 3 sensitized photo-oxidation of NADH in H2O/EtOH mixture with the intermediacy of singlet oxygen as judged by the effect of sodium azide on the photostimulated oxygen consumption. Evolution of O2 upon addition of catalase to the illuminated solution confirmed the ultimate formation of hydrogen peroxide. These findings suggested that the (di)amino-dimethoxyanthraquinones might exert photosensitization via both Type I and Type II mechanisms. The AAQs were tested for their ability to photosensitize K562 human chronic myeloid leukemic cells in culture. Viability was measured using the 3,4,5-diethylthiazol-2,5-diphenyl tetrazolium blue assay, and DNA and possible membrane damage were assessed. The results from illuminating cells with light > 475 nm show that for the 1,5-compounds, the presence of methoxy substituents at 4,8 positions reduces the dark toxicity from ID50 of 23 to 250 microM and for the 1,8-compounds correspondingly from ID50 of 53 to > 300 microM. In the 1,5-series this decrease of the dark toxicity is accompanied by an increase in light-induced dose modification from 8.85 to 14.4. Differences exist in the mechanisms of cytotoxicity between the prototype phenolic AAQs and their methoxy counterparts. It appears that the cytotoxic action of the latter causes cell damage by the formation of a high proportion of alkali labile sites in addition to frank strand breaks.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

本文描述了几种氨基蒽醌衍生物(AAQs)的合成,这些衍生物旨在抑制暗毒性并促进更高效的癌细胞光致敏作用,以用于光动力疗法(PDT)。合成了以下几种AAQs:1-NH₂-4,5-(MeO)₂-AQ(1)、1,5-(NH₂)₂-4,8-(MeO)₂-AQ(2)、1,8-(NH₂)₂-4,5-(MeO)₂-AQ(3)和1,5-(NHPhMe)₂-4,8-(MeO)₂-AQ(8)。这些试剂在480 - 620 nm区域表现出强烈吸收。通过测量1270 nm处的¹O₂磷光、采用电子顺磁共振(EPR)自旋捕获技术检测超氧自由基以及测量代表性生物电子供体NADH光氧化过程中的氧气消耗,研究了可能的光致敏机制。在苯中照射2和3时观察到¹O₂发出强烈磷光(在苯中的量子产率分别为0.25和0.5,在乙醇中的量子产率分别为0.23和0.34)。1-氨基-AQ(1)是最弱的¹O₂敏化剂,在苯中的量子产率为0.13,在乙醇中未观察到磷光。在1、2或3与5,5-二甲基-1-吡咯啉-N-氧化物(DMPO)的辐照苯溶液中,检测到超氧自由基作为DMPO的自旋加合物。根据叠氮化钠对光刺激的氧气消耗的影响判断,AAQs 2和3在H₂O/乙醇混合物中通过单线态氧介导使NADH发生光氧化。向光照溶液中加入过氧化氢酶后氧气的释放证实了最终形成了过氧化氢。这些发现表明(二)氨基二甲氧基蒽醌可能通过I型和II型机制发挥光致敏作用。测试了AAQs对培养的K562人慢性髓性白血病细胞进行光致敏的能力。使用3,4,5-二乙基噻唑-2,5-二苯基四氮唑蓝法测量细胞活力,并评估DNA和可能的膜损伤。用波长大于475 nm的光照射细胞的结果表明,对于1,5-化合物,4,8位存在甲氧基取代基可将暗毒性从ID50为23降低到250 μM,对于1,8-化合物相应地从ID50为53降低到大于300 μM。在1,5-系列中,暗毒性的这种降低伴随着光诱导剂量修正从8.85增加到14.4。原型酚类AAQs及其甲氧基类似物之间的细胞毒性机制存在差异。似乎后者的细胞毒性作用除了导致明显的链断裂外,还通过形成高比例的碱不稳定位点导致细胞损伤。(摘要截短至400字)

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