Discovery of a piperidine-4-carboxamide CCR5 antagonist (TAK-220) with highly potent anti-HIV-1 activity

Imamura S; Ichikawa T; Nishikawa Y; Kanzaki N; Takashima K; Niwa S; Iizawa Y; Baba M; Sugihara Y

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Discovery of a piperidine-4-carboxamide CCR5 antagonist (TAK-220) with highly potent anti-HIV-1 activity

机译：发现具有高效抗HIV-1活性的哌啶-4-羧酰胺CCR5拮抗剂（TAK-220）

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We incorporated various polar groups into previously described piperidine-4-carboxamide CCR5 antagonists to improve their metabolic stability in human hepatic microsomes. Introducing a carbamoyl group into the phenyl ring of the 4-benzylpiperidine moiety afforded the less lipophilic compound 5f, which possessed both high metabolic stability and good inhibitory activity of HIV-1 envelope-mediated membrane fusion (IC50 = 5.8 nM). Further optimization to increase potency led to the discovery of 1-acetyl-N-{3-[4-(4-carbamoylbenzyl) piperidin-1-yl]propyl}-N-(3-chloro-4-methylphenyl)piperidine-4-carboxamide (5m, TAK-220), which showed high CCR5 binding affinity (IC50 = 3.5 nM) and potent inhibition of membrane fusion (IC50 = 0.42 nM), as well as good metabolic stability. Compound 5m strongly inhibited the replication of CCR5-using HIV-1 clinical isolates in human peripheral blood mononuclear cells (mean EC50 = 1.1 nM, EC90 = 13 nM) and exhibited a good pharmacokinetic profile in monkeys (BA = 29%). This compound has been chosen as a clinical candidate for further development.

机译：我们将各种极性基团合并到先前描述的哌啶-4-羧酰胺CCR5拮抗剂中，以改善其在人肝微粒体中的代谢稳定性。将氨基甲酰基引入4-苄基哌啶部分的苯环中，得到的亲脂性较低的化合物5f既具有高代谢稳定性，又具有HIV-1包膜介导的膜融合的良好抑制活性（IC50 = 5.8 nM）。进一步优化以增加效力导致发现1-乙酰基-N- {3- [4-（4-氨基甲酰基苄基）哌啶-1-基]丙基} -N-（3-氯-4-甲基苯基）哌啶-4 -羧酰胺（5m，TAK-220），具有很高的CCR5结合亲和力（IC50 = 3.5 nM）和对膜融合的有效抑制（IC50 = 0.42 nM），以及良好的代谢稳定性。化合物5m强烈抑制使用HIV-1临床分离株的CCR5在人外周血单核细胞中的复制（平均EC50 = 1.1 nM，EC90 = 13 nM），并在猴子中表现出良好的药代动力学特征（BA = 29％）。该化合物已被选作进一步开发的临床候选药物。

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来源
《Journal of Medicinal Chemistry》 |2006年第9期|共10页
作者
Imamura S; Ichikawa T; Nishikawa Y; Kanzaki N; Takashima K; Niwa S; Iizawa Y; Baba M; Sugihara Y;
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正文语种 eng
中图分类药学;
关键词
BIOLOGICAL EVALUATION; HIV-1 INFECTION; SMALL-MOLECULE; DISEASE PROGRESSION; AGENTS; INDIVIDUALS; DERIVATIVES; GENE; AIDS; RESISTANCE;

机译：生物学评估;HIV-1感染;小分子;疾病进展;代理人;个人;衍生物;基因;艾滋病;抵抗力;

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1. Discovery of a piperidine-4-carboxamide CCR5 antagonist (TAK-220) with highly potent anti-HIV-1 activity [J] . Imamura S, Ichikawa T, Nishikawa Y, Journal of Medicinal Chemistry . 2006,第9期

机译：发现具有高效抗HIV-1活性的哌啶-4-羧酰胺CCR5拮抗剂（TAK-220）
2. Highly potent inhibition of human immunodeficiency virus type 1 replication by TAK-220, an orally bioavailable small-molecule CCR5 antagonist. [J] . Takashima K, Miyake H, Kanzaki N, Antimicrobial agents and chemotherapy. . 2005,第8期

机译：TAK-220是一种口服生物利用的小分子CCR5拮抗剂，对人类1型免疫缺陷病毒的复制具有高效抑制作用。
3. Highly Potent and Orally Active CCR5 Antagonists as Anti-HIV-1 Agents:Synthesis and Biological Activities of 1-Benzazocine Derivatives Containing a Sulfoxide Moiety [J] . Masaki Seto, Katsuji Aikawa, Naoki Miyamoto, Journal of Medicinal Chemistry . 2006,第6期

机译：高强度和口服活性的CCR5拮抗剂作为抗HIV-1剂：含有亚砜部分的1-苯并偶氮衍生物的合成和生物活性
4. Synthesis and pharmacological activity of Dmt-Tic analogs with highly potent agonist and antagonist/agonist opioid activity [C] . Remo Guerrini, Gianfranco Balboni, Daniela Girolamo Calo, the International Peptide Symposium . 2001

机译：具有高效激动剂和拮抗剂/激动剂阿片类能活性DMT-TIC类似物的合成与药理活性
5. Design, synthesis, and biological evaluation of betulinic acid derivatives as potent anti-HIV-1 agents. [D] . Qian, Keduo. 2008

机译：作为有效的抗HIV-1药物的桦木酸衍生物的设计，合成和生物学评估。
6. Discovery of INCB9471 a Potent Selective and Orally Bioavailable CCR5 Antagonist with Potent Anti-HIV-1 Activity [O] . Chu-Biao Xue, *, Lihua Chen, 2010

机译：发现具有有效抗HIV-1活性的有效选择性和口服生物利用CCR5拮抗剂INCB9471
7. Discovery of a Piperidine-4-carboxamide CCR5 Antagonist (TAK-220) with Highly Potent Anti-HIV-1 Activity [O] . -1

机译：发现哌啶-4-甲酰胺CCR5拮抗剂（TWA-220），具有高效的抗HIV-1活性

Discovery of a piperidine-4-carboxamide CCR5 antagonist (TAK-220) with highly potent anti-HIV-1 activity

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