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Novel bifunctional quinolonyl diketo acid derivatives as HIV-1 integrase inhibitors: Design, synthesis, biological activities, and mechanism of action

机译：作为HIV-1整合酶抑制剂的新型双功能喹啉基二酮酸衍生物：设计，合成，生物学活性和作用机理

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Novel quinolinonyl diketo acids were designed to obtain integrase (IN) inhibitors selectively active against the strand transfer (ST) step of the HIV integration process. Those new compounds are characterized by a single aryl diketo acid (DKA) chain in comparison to 4, a bifunctional diketo acid reported by our group as an anti-IN agent highly potent against both the 3'-processing and ST steps. Compound 6d was the most potent derivative in IN enzyme assays, while 6i showed the highest potency against HIV-1 in acutely infected cells. The selective inhibition of ST suggested the newly designed monofunctional DKAs bind the IN-DNA acceptor site without affecting the DNA donor site.

机译：设计新的喹啉酮基二酮酸以获得对HIV整合过程的链转移（ST）步骤有选择性的活性的整合酶（IN）抑制剂。与4相比，这些新化合物的特征是单芳基二酮酸（DKA）链，这是我们小组报告的双官能二酮酸，是一种抗3端加工和ST步骤的高效抗IN剂。化合物6d是IN酶测定中最有效的衍生物，而6i在急性感染的细胞中显示出对HIV-1的最高效力。对ST的选择性抑制表明，新设计的单功能DKA结合了IN-DNA受体位点而不影响DNA供体位点。

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Di Santo R; Costi R; Roux A; Artico M; Lavecchia A; Marinelli L; Novellino E; Palmisano L; Andreotti M; Amici R; Galluzzo C M; Nencioni L; Palamara A T; Pommier Y; Marchand C;
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1. Novel Bifunctional Quinolonyl Diketo Acid Derivatives as HIV-1 Integrase Inhibitors:Design,Synthesis,Biological Activities,and Mechanism of Action [J] . Roberto Di Santo, Roberta Costi, Alessandra Roux, Journal of Medicinal Chemistry . 2006,第6期

机译：新型双功能喹诺酮基二酮酸衍生物作为HIV-1整合酶抑制剂：设计，合成，生物活性和作用机理。
2. Novel quinolinonyl diketo acid derivatives as HIV-1 integrase inhibitors: Design, synthesis, and biological activities [J] . Di Santo R, Costi R, Roux A, Journal of Medicinal Chemistry . 2008,第15期

机译：新型喹啉酮基二酮酸衍生物作为HIV-1整合酶抑制剂：设计，合成和生物学活性
3. QSAR modeling of bifunctional quinolonyl diketo acid derivatives as integrase inhibitors [J] . Sonal Dubey, Nahid Abbas, G. Goutham, Medicinal Chemistry Research . 2012,第7期

机译：双功能喹诺酮基二酮酸衍生物作为整合酶抑制剂的QSAR建模
4. HIV-1 Integrase" Strand Transfer Inhibitors (INSTIs): Design, Synthesis and Biological Activity [C] . S. Ferro, M.L. Barreca, L. De Luca, Joint Meeting on Medicinal Chemistry . 2007

机译：HIV-1整合酶“链转移抑制剂（instis）：设计，合成和生物活性
5. Design and synthesis of molecular probes to modulate cell membrane permeation: I. Design, synthesis, and biological evaluation of novel chicoric acid analogues as inhibitors of HIV-1 integrase. II. Design, synthesis, and biological evaluation of novel estradiol analogues targeting the membrane estrogen receptor. [D] . Charvat, Trevor Thomas. 2004

机译：设计和合成的分子探针，可调节细胞膜的渗透性：I.设计，合成和生物评价作为抗HIV-1整合酶抑制剂的新型菊苣酸类似物。二。针对膜雌激素受体的新型雌二醇类似物的设计，合成和生物学评估。
6. Novel Bifunctional Quinolonyl Diketo Acid Derivatives as HIV-1 Integrase Inhibitors: Design Synthesis Biological Activities and Mechanism of Action [O] . Roberto Di Santo, Roberta Costi, Alessandra Roux, -1

机译：新型双功能喹诺酮基二酮酸衍生物作为HIV-1整合酶抑制剂：设计合成生物活性和作用机理。
7. Novel Bifunctional Quinolonyl Diketo Acid Derivatives as HIV-1 Integrase Inhibitors: Design, Synthesis, Biological Activities, and Mechanism of Action [O] . R. DI SANTO, R. COSTI, A. ROUX, 2006

机译：新型双功能喹啉基二酮酸衍生物作为HIV-1整合酶抑制剂：设计，合成，生物活性和作用机理

Novel bifunctional quinolonyl diketo acid derivatives as HIV-1 integrase inhibitors: Design, synthesis, biological activities, and mechanism of action

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