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Literature DB >> 19017562

Discovery and development of heat shock protein 90 inhibitors.

Tony Taldone¹, Weilin Sun, Gabriela Chiosis.

Abstract

Heat shock protein 90 (Hsp90) is an important target in cancer because of its role in maintaining transformation and has recently become the focus of several drug discovery and development efforts. While compounds with different modes of action are known, the focus of this review is on those classes of compounds which inhibit Hsp90 by binding to the N-terminal ATP pocket. These include natural product inhibitors such as geldanamycin and radicicol and synthetic inhibitors comprised of purines, pyrazoles, isoxazoles and other scaffolds. The synthetic inhibitors have been discovered either by structure-based design, high throughput screening and more recently using fragment-based design and virtual screening techniques. This review will discuss the discovery of these different classes, as well as their development as potential clinical agents.

Entities: CellLine Chemical Disease Gene Species

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Year: 2008 PMID： 19017562 PMCID： PMC2760286 DOI： 10.1016/j.bmc.2008.10.087

Source DB: PubMed Journal: Bioorg Med Chem ISSN： 0968-0896 Impact factor: 3.641

87 in total

1. Identification of potent water soluble purine-scaffold inhibitors of the heat shock protein 90.

Authors: Huazhong He; Danuta Zatorska; Joungnam Kim; Julia Aguirre; Laura Llauger; Yuhong She; Nian Wu; Robert M Immormino; Daniel T Gewirth; Gabriela Chiosis
Journal: J Med Chem Date: 2006-01-12 Impact factor: 7.446

2. Structure-based discovery of a new class of Hsp90 inhibitors.

Authors: Xavier Barril; Paul Brough; Martin Drysdale; Roderick E Hubbard; Andrew Massey; Allan Surgenor; Lisa Wright
Journal: Bioorg Med Chem Lett Date: 2005-10-03 Impact factor: 2.823

3. Activated B-RAF is an Hsp90 client protein that is targeted by the anticancer drug 17-allylamino-17-demethoxygeldanamycin.

Authors: Silvy da Rocha Dias; Frank Friedlos; Yvonne Light; Caroline Springer; Paul Workman; Richard Marais
Journal: Cancer Res Date: 2005-12-01 Impact factor: 12.701

4. Concise synthesis of pochonin A, an HSP90 inhibitor.

Authors: Emilie Moulin; Sofia Barluenga; Nicolas Winssinger
Journal: Org Lett Date: 2005-12-08 Impact factor: 6.005

5. 7'-substituted benzothiazolothio- and pyridinothiazolothio-purines as potent heat shock protein 90 inhibitors.

Authors: Lin Zhang; Junhua Fan; Khang Vu; Kevin Hong; Jean-Yves Le Brazidec; Jiandong Shi; Marco Biamonte; David J Busch; Rachel E Lough; Roy Grecko; Yingqing Ran; John L Sensintaffar; Adeela Kamal; Karen Lundgren; Francis J Burrows; Robert Mansfield; Gregg A Timony; Edgar H Ulm; Srinivas R Kasibhatla; Marcus F Boehm
Journal: J Med Chem Date: 2006-08-24 Impact factor: 7.446

6. 3-(5-Chloro-2,4-dihydroxyphenyl)-pyrazole-4-carboxamides as inhibitors of the Hsp90 molecular chaperone.

Authors: Paul A Brough; Xavier Barril; Mandy Beswick; Brian W Dymock; Martin J Drysdale; Lisa Wright; Kate Grant; Andrew Massey; Allan Surgenor; Paul Workman
Journal: Bioorg Med Chem Lett Date: 2005-10-05 Impact factor: 2.823

7. Design, synthesis, and biological evaluation of hydroquinone derivatives of 17-amino-17-demethoxygeldanamycin as potent, water-soluble inhibitors of Hsp90.

Authors: Jie Ge; Emmanuel Normant; James R Porter; Janid A Ali; Marlene S Dembski; Yun Gao; Asimina T Georges; Louis Grenier; Roger H Pak; Jon Patterson; Jens R Sydor; Thomas T Tibbitts; Jeffrey K Tong; Julian Adams; Vito J Palombella
Journal: J Med Chem Date: 2006-07-27 Impact factor: 7.446

8. Orally active purine-based inhibitors of the heat shock protein 90.

Authors: Marco A Biamonte; Jiandong Shi; Kevin Hong; David C Hurst; Lin Zhang; Junhua Fan; David J Busch; Patricia L Karjian; Angelica A Maldonado; John L Sensintaffar; Yong-Ching Yang; Adeela Kamal; Rachel E Lough; Karen Lundgren; Francis J Burrows; Gregg A Timony; Marcus F Boehm; Srinivas R Kasibhatla
Journal: J Med Chem Date: 2006-01-26 Impact factor: 7.446

Review 9. Targeting chaperones in transformed systems--a focus on Hsp90 and cancer.

Authors: Gabriela Chiosis
Journal: Expert Opin Ther Targets Date: 2006-02 Impact factor: 6.902

10. 4-Amino derivatives of the Hsp90 inhibitor CCT018159.

Authors: Xavier Barril; Mandy C Beswick; Adam Collier; Martin J Drysdale; Brian W Dymock; Alexandra Fink; Kate Grant; Robert Howes; Allan M Jordan; Andrew Massey; Allan Surgenor; Joanne Wayne; Paul Workman; Lisa Wright
Journal: Bioorg Med Chem Lett Date: 2006-02-09 Impact factor: 2.823

54 in total

Discovery and development of heat shock protein 90 inhibitors.

1. Identification of potent water soluble purine-scaffold inhibitors of the heat shock protein 90.

2. Structure-based discovery of a new class of Hsp90 inhibitors.

3. Activated B-RAF is an Hsp90 client protein that is targeted by the anticancer drug 17-allylamino-17-demethoxygeldanamycin.

4. Concise synthesis of pochonin A, an HSP90 inhibitor.

5. 7'-substituted benzothiazolothio- and pyridinothiazolothio-purines as potent heat shock protein 90 inhibitors.

6. 3-(5-Chloro-2,4-dihydroxyphenyl)-pyrazole-4-carboxamides as inhibitors of the Hsp90 molecular chaperone.

7. Design, synthesis, and biological evaluation of hydroquinone derivatives of 17-amino-17-demethoxygeldanamycin as potent, water-soluble inhibitors of Hsp90.

8. Orally active purine-based inhibitors of the heat shock protein 90.

Review 9. Targeting chaperones in transformed systems--a focus on Hsp90 and cancer.

10. 4-Amino derivatives of the Hsp90 inhibitor CCT018159.

1. Inhibition of heat-shock protein 90 reduces Ebola virus replication.

2. Impact of linker length on the activity of PROTACs.

Review 3. Comprehensive survey of chemical libraries for drug discovery and chemical biology: 2009.

4. Advances in the discovery and development of heat-shock protein 90 inhibitors for cancer treatment.

5. HSP90 functions in the circadian clock through stabilization of the client F-box protein ZEITLUPE.

Review 6. Advances in the clinical development of heat shock protein 90 (Hsp90) inhibitors in cancers.

7. The multiple roles of computational chemistry in fragment-based drug design.

8. Enforced N-domain proximity stimulates Hsp90 ATPase activity and is compatible with function in vivo.

Review 9. Molecular chaperones and regulation of tau quality control: strategies for drug discovery in tauopathies.

10. Modular control of cross-oligomerization: analysis of superstabilized Hsp90 homodimers in vivo.