Journal of Medicinal Chemistry

, volume 49 , issue 9 , pages 2784-2793

Discovery of a Piperidine-4-carboxamide CCR5 Antagonist (TAK-220) with Highly Potent Anti-HIV-1 Activity

Shinichi Imamura ¹

Takashi Ichikawa ¹

Youichi Nishikawa ¹

Naoyuki Kanzaki ¹

Katsunori Takashima ¹

Shinichi Niwa ¹

Yuji Iizawa ¹

Masanori Baba ¹

Yoshihiro SUGIHARA ¹

Hide authors affiliations Show authors affiliations: 1 affiliation

Pharmaceutical Research Division, Takeda Pharmaceutical Company Limited, 2-17-85, Jusohonmachi, Yodogawa-ku, Osaka 532-8686, Japan, and Division of Antiviral Chemotherapy, Center for Chronic Viral Diseases, Graduate School of Medical and Dental Sciences, Kagoshima University, 8-35-1, Sakuragaoka, Kagoshima 890-8544, Japan

Takeda Pharmaceutical Company

Kagoshima University

Publication type: Journal Article

Publication date: 2006-04-05

American Chemical Society (ACS)

Journal of Medicinal Chemistry

scimago Q1

wos Q1

SJR: 1.801

CiteScore: 11.5

Impact factor: 6.8

ISSN: 00222623, 15204804

DOI: 10.1021/jm051034q

Copy DOI

PubMed ID: 16640339

Drug Discovery

Molecular Medicine

Abstract

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 (IC(50) = 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 (IC(50) = 3.5 nM) and potent inhibition of membrane fusion (IC(50) = 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 EC(50) = 1.1 nM, EC(90) = 13 nM) and exhibited a good pharmacokinetic profile in monkeys (BA = 29%). This compound has been chosen as a clinical candidate for further development.

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GOST |

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GOST Copy

Imamura S. et al. Discovery of a Piperidine-4-carboxamide CCR5 Antagonist (TAK-220) with Highly Potent Anti-HIV-1 Activity // Journal of Medicinal Chemistry. 2006. Vol. 49. No. 9. pp. 2784-2793.

GOST all authors (up to 50) Copy

Imamura S., Ichikawa T., Nishikawa Y., Kanzaki N., Takashima K., Niwa S., Iizawa Y., Baba M., SUGIHARA Y. Discovery of a Piperidine-4-carboxamide CCR5 Antagonist (TAK-220) with Highly Potent Anti-HIV-1 Activity // Journal of Medicinal Chemistry. 2006. Vol. 49. No. 9. pp. 2784-2793.

RIS |

Cite this

RIS Copy

TY - JOUR

DO - 10.1021/jm051034q

UR - https://doi.org/10.1021/jm051034q

TI - Discovery of a Piperidine-4-carboxamide CCR5 Antagonist (TAK-220) with Highly Potent Anti-HIV-1 Activity

T2 - Journal of Medicinal Chemistry

AU - Imamura, Shinichi

AU - Ichikawa, Takashi

AU - Nishikawa, Youichi

AU - Kanzaki, Naoyuki

AU - Takashima, Katsunori

AU - Niwa, Shinichi

AU - Iizawa, Yuji

AU - Baba, Masanori

AU - SUGIHARA, Yoshihiro

PY - 2006

DA - 2006/04/05

PB - American Chemical Society (ACS)

SP - 2784-2793

IS - 9

VL - 49

PMID - 16640339

SN - 0022-2623

SN - 1520-4804

ER -

BibTex |

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BibTex (up to 50 authors) Copy

@article{2006_Imamura,

author = {Shinichi Imamura and Takashi Ichikawa and Youichi Nishikawa and Naoyuki Kanzaki and Katsunori Takashima and Shinichi Niwa and Yuji Iizawa and Masanori Baba and Yoshihiro SUGIHARA},

title = {Discovery of a Piperidine-4-carboxamide CCR5 Antagonist (TAK-220) with Highly Potent Anti-HIV-1 Activity},

journal = {Journal of Medicinal Chemistry},

year = {2006},

volume = {49},

publisher = {American Chemical Society (ACS)},

month = {apr},

url = {https://doi.org/10.1021/jm051034q},

number = {9},

pages = {2784--2793},

doi = {10.1021/jm051034q}

}

MLA

Cite this

MLA Copy

Imamura, Shinichi, et al. “Discovery of a Piperidine-4-carboxamide CCR5 Antagonist (TAK-220) with Highly Potent Anti-HIV-1 Activity.” Journal of Medicinal Chemistry, vol. 49, no. 9, Apr. 2006, pp. 2784-2793. https://doi.org/10.1021/jm051034q.

Publisher

American Chemical Society (ACS)

Journal

Journal of Medicinal Chemistry

scimago Q1

wos Q1

SJR

1.801

CiteScore

11.5

Impact factor

6.8

ISSN

00222623 (Print)

15204804 (Electronic)