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The in vitro ejection of zinc from human immunodeficiency virus (HIV) type 1 nucleocapsid protein by disulfide benzamides with cellular anti-HIV activity.

机译：具有细胞抗HIV活性的二硫苯甲酰胺体外从人免疫缺陷病毒（HIV）1型核衣壳蛋白中排出锌。

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Several disulfide benzamides have been shown to possess wide-spectrum antiretroviral activity in cell culture at low micromolar to submicromolar concentrations, inhibiting human immunodeficiency virus (HIV) type 1 (HIV-1) clinical and drug-resistant strains along with HIV-2 and simian immunodeficiency virus [Rice, W. G., Supko, J. G., Malspeis, L., Buckheit, R. W., Jr., Clanton, D., Bu, M., Graham, L., Schaeffer, C. A., Turpin, J. A., Domagala, J., Gogliotti, R., Bader, J. P., Halliday, S. M., Coren, L., Sowder, R. C., II, Arthur, L. O. & Henderson, L. E. (1995) Science 270, 1194-1197]. Rice and coworkers have proposed that the compounds act by "attacking" the two zinc fingers of HIV nucleocapsid protein. Shown here is evidence that low micromolar concentrations of the anti-HIV disulfide benzamides eject zinc from HIV nucleocapsid protein (NCp7) in vitro, as monitored by the zinc-specific fluorescent probe N-(6-methoxy-8-quinoyl)-p-toluenesulfonamide (TSQ). Structurally similar disulfide benzamides that do not inhibit HIV-1 in culture do not eject zinc, nor do analogs of the antiviral compounds with the disulfide replaced with a methylene sulfide. The kinetics of NCp7 zinc ejection by disulfide benzamides were found to be nonsaturable and biexponential, with the rate of ejection from the C-terminal zinc finger 7-fold faster than that from the N-terminal. The antiviral compounds were found to inhibit the zinc-dependent binding of NCp7 to HIV psi RNA, as studied by gel-shift assays, and the data correlated well with the zinc ejection data. Anti-HIV disulfide benzamides specifically eject NCp7 zinc and abolish the protein's ability to bind psi RNA in vitro, providing evidence for a possible antiretroviral mechanism of action of these compounds. Congeners of this class are under advanced preclinical evaluation as a potential chemotherapy for acquired immunodeficiency syndrome.

机译：已显示几种二硫化物苯甲酰胺在低微摩尔至亚微摩尔浓度的细胞培养物中具有广谱抗逆转录病毒活性，可抑制人类免疫缺陷病毒（HIV）1型（HIV-1）临床和耐药菌株以及HIV-2和猿猴免疫缺陷病毒[Rice，WG，Supko，JG，Malspeis，L.，Buckheit，RW，Jr.，Clanton，D.，Bu，M.，Graham，L.，Schaeffer，CA，Turpin，JA，Domagala，J. ，Gogliotti，R.，Bader，JP，Halliday，SM，Coren，L.，Sowder，RC，II，Arthur，LO＆Henderson，LE（1995）Science 270，1194-1197]。赖斯及其同事提出，这些化合物通过“攻击” HIV核衣壳蛋白的两个锌指起作用。此处显示的证据是，通过锌特异性荧光探针N-（6-甲氧基-8-喹啉基）-p-监测，低微摩尔浓度的抗HIV二硫化物苯甲酰胺体外可从HIV核衣壳蛋白（NCp7）喷出锌。甲苯磺酰胺（TSQ）。在结构上相似的，不抑制培养物中HIV-1的二硫化物苯甲酰胺不会喷射锌，二硫化物被亚甲基硫取代的抗病毒化合物的类似物也不会喷射锌。发现二硫化物苯甲酰胺排出NCp7锌的动力学是不饱和的并且是双指数的，从C端锌指的排出速率比从N端快7倍。如通过凝胶位移分析所研究的，发现抗病毒化合物抑制NCp7与HIV psi RNA的锌依赖性结合，并且该数据与锌排出数据很好地相关。抗HIV二硫化物苯甲酰胺特异地排出NCp7锌，并取消了该蛋白在体外结合psi RNA的能力，为这些化合物可能的抗逆转录病毒作用机理提供了证据。同类同类药物正在接受临床前评估，作为获得性免疫缺陷综合症的潜在化学疗法。

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Tummino, P J; Scholten, J D; Harvey, P J; Holler, T P; Maloney, L; Gogliotti, R; Domagala, J; Hupe, D;
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年度 1996
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1. The in vitro ejection of zinc from human immunodeficiency virus (HIV) type 1 nucleocapsid protein by disulfide benzamides with cellular anti-HIV activity [J] . Peter J. Tummino, Jeffrey D. Scholten, Patricia J. Harvey Proceedings of the National Academy of Sciences of the United States of America . 1996 ,第3期

机译：具有细胞抗HIV活性的二硫苯甲酰胺体外从人免疫缺陷病毒（HIV）1型核衣壳蛋白中排出锌
2. EFFECT OF HUMAN IMMUNODEFICIENCY VIRUS TYPE 1 (HIV-1) NUCLEOCAPSID PROTEIN ON HIV-1 REVERSE TRANSCRIPTASE ACTIVITY IN VITRO [J] . Ji XD, Klarmann GJ, Preston BD Biochemistry . 1996 ,第1期

机译：人类免疫缺陷病毒1型（HIV-1）核衣壳蛋白对HIV-1逆转录酶活性的体外影响
3. INHIBITION OF THE INTEGRASE OF HUMAN IMMUNODEFICIENCY VIRUS (HIV) TYPE 1 BY ANTI-HIV PLANT PROTEINS MAP30 AND GAP31 [J] . Leehuang S., Huang PL., Bourinbaiar AS., Proceedings of the National Academy of Sciences of the United States of America . 1995 ,第19期

机译：抗HIV植物蛋白MAP30和GAP31抑制1型人类免疫缺陷病毒（HIV）的整合
4. RAPID AND SENSITIVE DETECTION OF CAPSID PROTEIN P24 OF HUMAN IMMUNODEFICIENCY VIRUS TYPE 1 (HIV-1) USING ON-CHIP EUROPIUM (III) NANOPARTICLE-BASED IMMUNOASSAY [C] . J. Liu, B. Du, S. Tang, International Conference on Miniaturized Systems for Chemistry and Life Sciences . 2011

机译：使用片上铕（III）纳米粒子类免疫测定的人免疫缺陷病毒型1（HIV-1）的人体免疫缺陷病毒病毒病毒型（HIV-1）的快速敏感检测
5. Human immunodeficiency virus nucleocapsid protein: Analysis of the mechanism of strand exchange and the role of the zinc fingers in nucleic acid chaperone activity. [D] . Heath, Megan Joy. 2004

机译：人类免疫缺陷病毒核衣壳蛋白：链交换机制和锌指在核酸伴侣活性中的作用分析。
6. The in vitro ejection of zinc from human immunodeficiency virus (HIV) type 1 nucleocapsid protein by disulfide benzamides with cellular anti-HIV activity. [O] . P J Tummino, J D Scholten, P J Harvey, 1996

机译：具有细胞抗HIV活性的二硫苯甲酰胺体外从人免疫缺陷病毒（HIV）1型核衣壳蛋白中排出锌。
7. Human Cellular Nucleic Acid-Binding Protein Zn2+ Fingers Support Replication of Human Immunodeficiency Virus Type 1 When They Are Substituted in the Nucleocapsid Protein [O] . McGrath, Connor F., Buckman, James S., Gagliardi, Tracy D., 2003

机译：人类细胞核酸结合蛋白Zn2 +手指替代人免疫缺陷病毒1型时，支持复制它们在Nucleoppsid蛋白中。
8. Human Immunodeficiency Virus Type 1 (HIV-1) Viral Protein R (Vpr)- Mediated Cell Cycle Arrest: An Analysis of Current Mechanistic Models [R] . Sercovich, M. J. 2006

机译：人类免疫缺陷病毒1型（HIV-1）病毒蛋白R（Vpr） - 介导的细胞周期逮捕：当前机制模型的分析

The in vitro ejection of zinc from human immunodeficiency virus (HIV) type 1 nucleocapsid protein by disulfide benzamides with cellular anti-HIV activity.

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