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对肿瘤、病毒和细菌有活性的多金属氧酸盐。

Polyoxometalates active against tumors, viruses, and bacteria.

作者信息

Yamase Toshihiro

机构信息

MO device, 2-14-10 Kanaiwa-higashi, Kanazawa, 920-0335, Japan,

出版信息

Prog Mol Subcell Biol. 2013;54:65-116. doi: 10.1007/978-3-642-41004-8_4.

Abstract

Polyoxometalates (PMs) as discrete metal-oxide cluster anions with high solubility in water and photochemically and electrochemically active property have a wide variety of structures not only in molecular size from sub-nano to sub-micrometers with a various combination of metals but also in symmetry and highly negative charge. One of the reasons for such a structural variety originates from their conformation change (due to the condensed aggregation and the structural assembly) which strongly depends on environmental parameters such as solution pH, concentration, and coexistent foreign inorganic and/or organic substances. In the course of the application of the physicochemical properties of such PMs to the medical fields, antitumoral, antiviral, and antibacterial activities have been developed for realization of a novel inorganic medicine which provides a biologically excellent activity never replaced by other approved medicines. Several PMs as a candidate for clinical uses have been licensed toward the chemotherapy of solid tumors (such as human gastric cancer and pancreatic cancer), DNA and RNA viruses (such as HSV, HIV, influenza, and SARS), and drug-resistant bacteria (such as MRSA and VRSA) in recent years: [NH3Pr(i)]6[Mo7O24]∙3H2O (PM-8) and [Me3NH]6[H2Mo(V) 12O28(OH)12(Mo(VI)O3)4]∙2H2O (PM-17) for solid tumors; K7[PTi2W10O40]∙6H2O (PM-19), [Pr(i)NH3]6H[PTi2W10O38(O2)2]∙H2O (PM-523), and K11H[(VO)3(SbW9O33)2]∙27H2O (PM-1002) for viruses; and K6[P2W18O62]∙14H2O (PM-27), K4[SiMo12O40]∙3H2O (SiMo12), and PM-19 for MRSA and VRSA. The results are discussed from a point of view of the chemotherapeutic clarification in this review.

摘要

多金属氧酸盐(PMs)作为离散的金属氧化物簇阴离子,在水中具有高溶解性,且具有光化学和电化学活性,不仅在分子尺寸上从亚纳米到亚微米不等,金属组合多样,而且在对称性和高负电荷方面也具有多种结构。这种结构多样性的原因之一源于它们的构象变化(由于缩合聚集和结构组装),这强烈依赖于环境参数,如溶液pH值、浓度以及共存的外来无机和/或有机物质。在将此类PMs的物理化学性质应用于医学领域的过程中,已经开发出了抗肿瘤、抗病毒和抗菌活性,以实现一种新型无机药物,该药物具有其他已批准药物无法替代的优异生物学活性。近年来,几种作为临床应用候选药物的PMs已被批准用于实体瘤(如人类胃癌和胰腺癌)、DNA和RNA病毒(如单纯疱疹病毒、艾滋病毒、流感病毒和严重急性呼吸综合征病毒)以及耐药细菌(如耐甲氧西林金黄色葡萄球菌和耐万古霉素金黄色葡萄球菌)的化疗:用于实体瘤的[NH3Pr(i)]6[Mo7O24]∙3H2O(PM - 8)和[Me3NH]6[H2Mo(V)12O28(OH)12(Mo(VI)O3)4]∙2H2O(PM - 17);用于病毒的K7[PTi2W10O40]∙6H2O(PM - 19)、[Pr(i)NH3]6H[PTi2W10O38(O2)2]∙H2O(PM - 523)和K11H[(VO)3(SbW9O33)2]∙27H2O(PM - 1002);用于耐甲氧西林金黄色葡萄球菌和耐万古霉素金黄色葡萄球菌的K6[P2W18O62]∙14H2O(PM - 27)、K4[SiMo12O40]∙3H2O(硅钼酸12)和PM - 19。本文将从化疗阐明的角度对这些结果进行讨论。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c0a5/7122307/5b1cdd804338/272275_1_En_4_Fig1_HTML.jpg

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