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- Publisher Website: 10.1021/jm400380m
- Scopus: eid_2-s2.0-84881425734
- PMID: 23829549
- WOS: WOS:000323082400006
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Article: The discovery of PLK4 inhibitors: (E)-3-((1H-indazol-6-yl)methylene) indolin-2-ones as novel antiproliferative agents
| Title | The discovery of PLK4 inhibitors: (E)-3-((1H-indazol-6-yl)methylene) indolin-2-ones as novel antiproliferative agents |
|---|---|
| Authors | Laufer, RadoslawForrest, BryanLi, Sze WanLiu, YongSampson, PeterEdwards, LouiseLang, YunhuiAwrey, Donald E.Mao, GuodongPlotnikova, OlgaLeung, GenieHodgson, RichardBeletskaya, IrinaMason, Jacqueline M.Luo, XunyiWei, XinYao, YiFeher, MiklosBan, FuqiangKiarash, RezaGreen, ErinMak, Tak W.Pan, GuohuaPauls, Henry W. |
| Issue Date | 2013 |
| Citation | Journal of Medicinal Chemistry, 2013, v. 56, n. 15, p. 6069-6087 How to Cite? |
| Abstract | The family of Polo-like kinases is important in the regulation of mitotic progression; this work keys on one member, namely Polo-like kinase 4 (PLK4). PLK4 has been identified as a candidate anticancer target which prompted a search for potent and selective inhibitors of PLK4. The body of the paper describes lead generation and optimization work which yielded nanomolar PLK4 inhibitors. Lead generation began with directed virtual screening, using a ligand-based focused library and a PLK4 homology model. Validated hits were used as starting points for the design and discovery of PLK4 inhibitors of novel structure, namely (E)-3-((1H-indazol-6-yl)methylene)indolin-2-ones. Computational models, based on a published X-ray structure (PLK4 kinase domain), were used to understand and optimize the in vitro activity of the series; potent antiproliferative activity was obtained. The kinase selectivity profile and cell cycle analysis of selected inhibitors are described. The results of a xenograft study with an optimized compound 50 (designated CFI-400437) support the potential of these novel PLK4 inhibitors for cancer therapy. © 2013 American Chemical Society. |
| Persistent Identifier | http://hdl.handle.net/10722/292767 |
| ISSN | 2023 Impact Factor: 6.8 2023 SCImago Journal Rankings: 1.986 |
| ISI Accession Number ID |
| DC Field | Value | Language |
|---|---|---|
| dc.contributor.author | Laufer, Radoslaw | - |
| dc.contributor.author | Forrest, Bryan | - |
| dc.contributor.author | Li, Sze Wan | - |
| dc.contributor.author | Liu, Yong | - |
| dc.contributor.author | Sampson, Peter | - |
| dc.contributor.author | Edwards, Louise | - |
| dc.contributor.author | Lang, Yunhui | - |
| dc.contributor.author | Awrey, Donald E. | - |
| dc.contributor.author | Mao, Guodong | - |
| dc.contributor.author | Plotnikova, Olga | - |
| dc.contributor.author | Leung, Genie | - |
| dc.contributor.author | Hodgson, Richard | - |
| dc.contributor.author | Beletskaya, Irina | - |
| dc.contributor.author | Mason, Jacqueline M. | - |
| dc.contributor.author | Luo, Xunyi | - |
| dc.contributor.author | Wei, Xin | - |
| dc.contributor.author | Yao, Yi | - |
| dc.contributor.author | Feher, Miklos | - |
| dc.contributor.author | Ban, Fuqiang | - |
| dc.contributor.author | Kiarash, Reza | - |
| dc.contributor.author | Green, Erin | - |
| dc.contributor.author | Mak, Tak W. | - |
| dc.contributor.author | Pan, Guohua | - |
| dc.contributor.author | Pauls, Henry W. | - |
| dc.date.accessioned | 2020-11-17T14:57:10Z | - |
| dc.date.available | 2020-11-17T14:57:10Z | - |
| dc.date.issued | 2013 | - |
| dc.identifier.citation | Journal of Medicinal Chemistry, 2013, v. 56, n. 15, p. 6069-6087 | - |
| dc.identifier.issn | 0022-2623 | - |
| dc.identifier.uri | http://hdl.handle.net/10722/292767 | - |
| dc.description.abstract | The family of Polo-like kinases is important in the regulation of mitotic progression; this work keys on one member, namely Polo-like kinase 4 (PLK4). PLK4 has been identified as a candidate anticancer target which prompted a search for potent and selective inhibitors of PLK4. The body of the paper describes lead generation and optimization work which yielded nanomolar PLK4 inhibitors. Lead generation began with directed virtual screening, using a ligand-based focused library and a PLK4 homology model. Validated hits were used as starting points for the design and discovery of PLK4 inhibitors of novel structure, namely (E)-3-((1H-indazol-6-yl)methylene)indolin-2-ones. Computational models, based on a published X-ray structure (PLK4 kinase domain), were used to understand and optimize the in vitro activity of the series; potent antiproliferative activity was obtained. The kinase selectivity profile and cell cycle analysis of selected inhibitors are described. The results of a xenograft study with an optimized compound 50 (designated CFI-400437) support the potential of these novel PLK4 inhibitors for cancer therapy. © 2013 American Chemical Society. | - |
| dc.language | eng | - |
| dc.relation.ispartof | Journal of Medicinal Chemistry | - |
| dc.title | The discovery of PLK4 inhibitors: (E)-3-((1H-indazol-6-yl)methylene) indolin-2-ones as novel antiproliferative agents | - |
| dc.type | Article | - |
| dc.description.nature | link_to_subscribed_fulltext | - |
| dc.identifier.doi | 10.1021/jm400380m | - |
| dc.identifier.pmid | 23829549 | - |
| dc.identifier.scopus | eid_2-s2.0-84881425734 | - |
| dc.identifier.volume | 56 | - |
| dc.identifier.issue | 15 | - |
| dc.identifier.spage | 6069 | - |
| dc.identifier.epage | 6087 | - |
| dc.identifier.eissn | 1520-4804 | - |
| dc.identifier.isi | WOS:000323082400006 | - |
| dc.identifier.issnl | 0022-2623 | - |