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Research Article

PI-273, a substrate-competitive, specific small molecule inhibitor of PI4KIIα, inhibits the growth of breast cancer cells

Jiangmei Li, Zhen Gao, Dan Zhao, lunfeng zhang, Xinhua Qiao, yingying zhao, Hong Ding, Panpan Zhang, Junyan Lu, Jia Liu, Hualiang Jiang, Cheng Luo and Chang Chen
Jiangmei Li
1National Laboratory of Biomacromolecules, Institute of Biophysics
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Zhen Gao
2Institute of Biophysics
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Dan Zhao
3Drug Discovery and Design Center, Shanghai Institute of Material Medica
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lunfeng zhang
2Institute of Biophysics
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Xinhua Qiao
2Institute of Biophysics
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yingying zhao
4SIAIS, Shanghaitech university
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Hong Ding
5State Key Laboratory of Drug Research, Shanghai Institute of Materia Medica
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Panpan Zhang
6Shanghaitech university
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Junyan Lu
7European Molecular Biology Laboratory
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Jia Liu
8Shanghaitech University
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Hualiang Jiang
3Drug Discovery and Design Center, Shanghai Institute of Material Medica
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Cheng Luo
3Drug Discovery and Design Center, Shanghai Institute of Material Medica
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Chang Chen
9National Laboratory of Biomacromolecules, Institute of Biophysics, Chinese Academy of Sciences
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  • For correspondence: changchen@moon.ibp.ac.cn
DOI: 10.1158/0008-5472.CAN-17-0484
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Abstract

While phosphatidylinositol 4-kinase PI4KIIα has been identified as a potential target for antitumor therapy, the clinical applications of PI4KIIα are limited by a lack of specific inhibitors. Here we report the first small-molecule inhibitor (SMI) of human PI4KIIα. Docking-based and ligand-based virtual screening strategies were first employed to identify promising hits, followed by two rounds of kinase activity inhibition validation. 2-(3-(4-Chlorobenzoyl)thioureido)-4-ethyl-5-methylthiophene-3-carboxamide (PI-273) exhibited the greatest inhibitory effect on PI4KIIα kinase activity (IC50 = 0.47 μM) and suppressed cell proliferation. Surface plasmon resonance (SPR) and thermal shift assays indicated that PI-273 interacted directly with PI4KIIα. Kinetic analysis identified PI-273 as a reversible competitive inhibitor with respect to the substrate phosphatidylinositol (PI), which contrasted with most other PI kinase inhibitors that bind the ATP binding site. PI-273 reduced PI4P content, cell viability, and AKT signaling in wild-type MCF-7 cells but not in PI4KIIα knockout MCF-7 cells, indicating that PI-273 is highly selective for PI4KIIα. Mutant analysis revealed a role of palmitoylation insertion in the selectivity of PI-273 for PI4KIIα. Additionally, PI-273 treatment retarded cell proliferation by blocking cells in G2/M, inducing cell apoptosis and suppressing colony-forming ability. Importantly, PI-273 significantly inhibited MCF-7 cell-induced breast tumor growth without toxicity. PI-273 is the first substrate-competitive, subtype-specific inhibitor of PI4KIIα, the use of which will facilitate evaluations of PI4KIIα as a cancer therapeutic target.

  • Received February 22, 2017.
  • Revision received June 29, 2017.
  • Accepted August 14, 2017.
  • Copyright ©2017, American Association for Cancer Research.
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Published OnlineFirst August 21, 2017
doi: 10.1158/0008-5472.CAN-17-0484

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PI-273, a substrate-competitive, specific small molecule inhibitor of PI4KIIα, inhibits the growth of breast cancer cells
Jiangmei Li, Zhen Gao, Dan Zhao, lunfeng zhang, Xinhua Qiao, yingying zhao, Hong Ding, Panpan Zhang, Junyan Lu, Jia Liu, Hualiang Jiang, Cheng Luo and Chang Chen
Cancer Res August 21 2017 DOI: 10.1158/0008-5472.CAN-17-0484

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PI-273, a substrate-competitive, specific small molecule inhibitor of PI4KIIα, inhibits the growth of breast cancer cells
Jiangmei Li, Zhen Gao, Dan Zhao, lunfeng zhang, Xinhua Qiao, yingying zhao, Hong Ding, Panpan Zhang, Junyan Lu, Jia Liu, Hualiang Jiang, Cheng Luo and Chang Chen
Cancer Res August 21 2017 DOI: 10.1158/0008-5472.CAN-17-0484
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