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Literature DB >> 18293999

Development of novobiocin analogues that manifest anti-proliferative activity against several cancer cell lines.

Joseph A Burlison¹, Christopher Avila, George Vielhauer, Donna J Lubbers, Jeffrey Holzbeierlein, Brian S J Blagg.

Abstract

Recent studies have shown that the DNA gyrase inhibitor, novobiocin, binds to a previously unrecognized ATP-binding site located at the C-terminus of Hsp90 and induces degradation of Hsp90-dependent client proteins at approximately 700 microM. As a result of these studies, several analogues of the coumarin family of antibiotics have been reported and shown to exhibit increased Hsp90 inhibitory activity; however, the monomeric species lacked the ability to manifest anti-proliferative activity against cancer cell lines at concentrations tested. In an effort to develop more efficacious compounds that produce growth inhibitory activity against cancer cell lines, structure-activity relationships were investigated surrounding the prenylated benzamide side chain of the natural product. Results obtained from these studies have produced the first novobiocin analogues that manifest anti-proliferative activity against several cancer cell lines.

Entities: Chemical Disease Gene

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Year: 2008 PMID： 18293999 DOI： 10.1021/jo702191a

Source DB: PubMed Journal: J Org Chem ISSN： 0022-3263 Impact factor: 4.354

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Cited

54 in total

1. Alternative approaches to Hsp90 modulation for the treatment of cancer.

Authors: Jessica A Hall; Leah K Forsberg; Brian S J Blagg
Journal: Future Med Chem Date: 2014-09 Impact factor: 3.808

2. Synthesis and evaluation of novologues as C-terminal Hsp90 inhibitors with cytoprotective activity against sensory neuron glucotoxicity.

Authors: Bhaskar Reddy Kusuma; Liang Zhang; Teather Sundstrom; Laura B Peterson; Rick T Dobrowsky; Brian S J Blagg
Journal: J Med Chem Date: 2012-06-15 Impact factor: 7.446

3. Synthesis and structure-activity relationships of EGCG analogues, a recently identified Hsp90 inhibitor.

Authors: Anuj Khandelwal; Jessica A Hall; Brian S J Blagg
Journal: J Org Chem Date: 2013-08-01 Impact factor: 4.354

Review 4. Anticancer Inhibitors of Hsp90 Function: Beyond the Usual Suspects.

Authors: Gaurav Garg; Anuj Khandelwal; Brian S J Blagg
Journal: Adv Cancer Res Date: 2016-02-10 Impact factor: 6.242

5. KU675, a Concomitant Heat-Shock Protein Inhibitor of Hsp90 and Hsc70 that Manifests Isoform Selectivity for Hsp90α in Prostate Cancer Cells.

Authors: Weiya Liu; George A Vielhauer; Jeffrey M Holzbeierlein; Huiping Zhao; Suman Ghosh; Douglas Brown; Eugene Lee; Brian S J Blagg
Journal: Mol Pharmacol Date: 2015-05-04 Impact factor: 4.436

6. Trifunctional High-Throughput Screen Identifies Promising Scaffold To Inhibit Grp94 and Treat Myocilin-Associated Glaucoma.

Authors: Dustin J E Huard; Vincent M Crowley; Yuhong Du; Ricardo A Cordova; Zheying Sun; Moya O Tomlin; Chad A Dickey; John Koren; Laura Blair; Haian Fu; Brian S J Blagg; Raquel L Lieberman
Journal: ACS Chem Biol Date: 2018-02-20 Impact factor: 5.100

Development of novobiocin analogues that manifest anti-proliferative activity against several cancer cell lines.

1. Alternative approaches to Hsp90 modulation for the treatment of cancer.

2. Synthesis and evaluation of novologues as C-terminal Hsp90 inhibitors with cytoprotective activity against sensory neuron glucotoxicity.

3. Synthesis and structure-activity relationships of EGCG analogues, a recently identified Hsp90 inhibitor.

Review 4. Anticancer Inhibitors of Hsp90 Function: Beyond the Usual Suspects.

5. KU675, a Concomitant Heat-Shock Protein Inhibitor of Hsp90 and Hsc70 that Manifests Isoform Selectivity for Hsp90α in Prostate Cancer Cells.

6. Trifunctional High-Throughput Screen Identifies Promising Scaffold To Inhibit Grp94 and Treat Myocilin-Associated Glaucoma.

7. Synthesis and evaluation of a ring-constrained Hsp90 C-terminal inhibitor that exhibits neuroprotective activity.

8. Exploiting polarity and chirality to probe the Hsp90 C-terminus.

Review 9. Novobiocin and additional inhibitors of the Hsp90 C-terminal nucleotide-binding pocket.

10. Synthesis and biological evaluation of coumarin replacements of novobiocin as Hsp90 inhibitors.