4.7 Article

Broad spectrum anti-RNA virus activities of titanium and vanadium substituted polyoxotungstates

期刊

ANTIVIRAL RESEARCH
卷 58, 期 3, 页码 265-271

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ELSEVIER SCIENCE BV
DOI: 10.1016/S0166-3542(03)00009-3

关键词

polyoxometalate; antiviral; RNA virus; HIV; Dengue fever virus

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Seven polyoxotungstates substituted with vanadium or titanium atoms were examined for their activity against Flaviviridae (Dengue fever virus. DFV), Orthomyxoviridae (influenza virus type A, fluV-A), Paramyxoviridae (respiratory syncytial virus, RSV, parainfluenza virus type 2, PfluV-2 and canine distemper virus, CDV) and Lentiviridae (human immunodeficiency virus type 1, HIV-1) families. Among the seven polyoxotungstates examined, PM-43 {K-5[SiVW11O40]}, PM-47 {K-7[BVW11O40]}, and PM-1001 [K10Na(VO)(3)(SbW9O33)(2)]26H(2)O contained vanadium. PM-1002 had the same core structure of (VO)(3)(SbW9O33)(2) as PM-1001; however, three V atoms of PM-1001 consisted of two V-IV and one V-V and those of PM-1002 consisted of three V-IV. On the other hand, PM-518 {[Et2NH2](7)[PTi2W10O40]}, PM-520 [Pri(2)NH(2)](5)[PTiW11O40] and PM-523 [PriNH(3)](6)H[PTi2W10O38(O-2)(2)]H2O all contained titanium. All compounds showed broad spectrum antiviral activity against all viruses examined except for PMs-43, -518 and -523 which did not exhibit inhibitory activity at greater than or equal to50 muM against PfluV-2. CDV and DFV, respectively. All compounds were inhibitory against HIV replication at an EC50 of less than 2.0 muM. Among them, PMs-1001 and -1002 showed the most potent inhibition. The compounds were not toxic for MDCK, HEp-2 and Vero cells at a concentration of 200 muM. For the exponentially growing MT-4 cells, the vanadium containing polyoxometalates (PMs-43, 47, 1001, 1002) showed toxicity at concentrations between 41 and 47 muM. On the other hand, titanium containing polyoxometalates (PMs-518, -520,-523) were not toxic at 100 muM. The mechanism of anti-HIV action of PM-1001 was analyzed: it affected the binding of HIV to the cell membrane and syncytium formation between HIV-infected and uninfected cells. (C) 2003 Elsevier Science B.V. All rights reserved.

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