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镓配合物作为抗癌药物

Gallium Complexes as Anticancer Drugs.

作者信息

Chitambar Christopher R

出版信息

Met Ions Life Sci. 2018 Feb 5;18. doi: 10.1515/9783110470734-016.

DOI:10.1515/9783110470734-016
PMID:29394029
Abstract

Clinical trials have shown gallium nitrate, a group 13 (formerly IIIa) metal salt, to have antineoplastic activity against non-Hodgkin's lymphoma and urothelial cancers. Interest in gallium as a metal with anticancer properties emerged when it was discovered that 67Ga(III) citrate injected in tumor-bearing animals localized to sites of tumor. Animal studies showed non-radioactive gallium nitrate to inhibit the growth of implanted solid tumors. Following further evaluation of its efficacy and toxicity in animals, gallium nitrate, Ga(NO3)3, was designated an investigational drug by the National Cancer Institute (USA) and advanced to Phase 1 and 2 clinical trials. Gallium(III) shares certain chemical characteristics with iron(III) which enable it to interact with iron-binding proteins and disrupt iron-dependent tumor cell growth. Gallium's mechanisms of action include the inhibition of cellular iron uptake and disruption of intracellular iron homeostasis, these effects result in inhibition of ribonucleotide reductase and mitochondrial function, and changes in the expression in proteins of iron transport and storage. Whereas the growth-inhibitory effects of gallium become apparent after 24 to 48 hours of incubation of cells, an increase in intracellular reactive oxygen species (ROS) is seen with 1 to 4 hours of incubation. Gallium-induced ROS consequently triggers the upregulation of metallothionein and hemoxygenase-1 genes. Beyond the first generation of gallium salts such as gallium nitrate and gallium chloride, a new generation of gallium-ligand complexes such as tris(8-quinolinolato)gallium(III) (KP46) and gallium maltolate has emerged. These agents are being evaluated in the clinic while other ligands for gallium are in preclinical development. These newer agents appear to possess greater antitumor efficacy and a broader spectrum of antineoplastic activity than the earlier generation of gallium compounds.

摘要

临床试验表明,13族(原IIIA族)金属盐硝酸镓对非霍奇金淋巴瘤和尿路上皮癌具有抗肿瘤活性。当发现将柠檬酸镓67Ga(III)注入荷瘤动物体内后会定位于肿瘤部位时,人们开始对具有抗癌特性的金属镓产生兴趣。动物研究表明,非放射性硝酸镓可抑制植入实体瘤的生长。在对其在动物体内的疗效和毒性进行进一步评估后,硝酸镓(Ga(NO3)3)被美国国立癌症研究所指定为研究性药物,并进入1期和2期临床试验。镓(III)与铁(III)具有某些化学特性,这使其能够与铁结合蛋白相互作用并破坏铁依赖性肿瘤细胞的生长。镓的作用机制包括抑制细胞对铁的摄取和破坏细胞内铁稳态,这些作用导致核糖核苷酸还原酶和线粒体功能受到抑制,以及铁运输和储存蛋白的表达发生变化。镓的生长抑制作用在细胞孵育24至48小时后变得明显,而在孵育1至4小时后可观察到细胞内活性氧(ROS)增加。镓诱导的ROS进而触发金属硫蛋白和血红素加氧酶-1基因的上调。除了第一代镓盐如硝酸镓和氯化镓之外,新一代镓-配体复合物如三(8-羟基喹啉)镓(III)(KP46)和苹果酸镓已经出现。这些药物正在临床中进行评估,而其他镓配体正处于临床前开发阶段。与早期的镓化合物相比,这些新型药物似乎具有更高的抗肿瘤疗效和更广泛的抗肿瘤活性谱。

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