Journal ArticleDOI
Inhibition of HSP90 molecular chaperones: moving into the clinic.
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TLDR
The current status of HSP90 inhibitors in clinical development is reviewed, including geldanamycin derivatives, resorcinol derivatives, purine analogues, and other synthetic inhibitors.Abstract:
Summary Heat shock protein 90 (HSP90) is a molecular chaperone that is crucial for the stability and function of many proteins essential for cell survival. Many oncogenes, including tyrosine kinases, transcription factors, and cell-cycle regulatory proteins, are client proteins of HSP90. Inhibition of HSP90 causes client protein degradation via the ubiquitin–proteasome pathway, and is a mechanism that might simultaneously downregulate several redundant pathways crucial for cell viability and tumour development. HSP90 inhibitors are currently being developed as anticancer agents, and have shown early promising results in molecularly defined subgroups of solid tumours (eg, ALK-rearranged non-small-cell lung cancer and HER2-amplified breast cancer) and some haematological malignancies (eg, multiple myeloma). Here, we review the current status of HSP90 inhibitors in clinical development, including geldanamycin derivatives, resorcinol derivatives, purine analogues, and other synthetic inhibitors. We also discuss novel strategies and future perspectives on how to optimise the therapeutic potential of this exciting new class of drugs.read more
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Journal ArticleDOI
Development of Heat Shock Protein (Hsp90) Inhibitors To Combat Resistance to Tyrosine Kinase Inhibitors through Hsp90-Kinase Interactions.
Meining Wang,Aijun Shen,Chi Zhang,Zilan Song,Jing Ai,Hongchun Liu,Li-Ping Sun,Jian Ding,Meiyu Geng,Ao Zhang +9 more
TL;DR: The objectives of the current perspective are to summarize the structure and function of the Hsp90-cochaperone-client complex, to analyze the structural and functional insights into the H Sp90-client interactions, and to highlight the preclinical and clinical studies of HSp90 inhibitors as an effective treatment against resistance to tyrosine kinase inhibitors.
Journal ArticleDOI
Molecular Chaperones of Leishmania: Central Players in Many Stress-Related and -Unrelated Physiological Processes
TL;DR: Heat shock proteins play important roles in adaptation and survival of this parasite against temperature changes associated with its passage from the poikilothermic insect vector to the warm-blooded vertebrate host.
Journal ArticleDOI
Clusterin facilitates metastasis by EIF3I/Akt/MMP13 signaling in hepatocellular carcinoma.
Cun Wang,Guangzhi Jin,Haojie Jin,Ning Wang,Qin Luo,Yurong Zhang,Dong-Mei Gao,Kai Jiang,Dishui Gu,Qiujing Shen,Xisong Huo,Fangyuan Hu,Tianxiang Ge,Fangyu Zhao,Wei Chu,Huiqun Shu,Ming Yao,Wenming Cong,Wenxin Qin +18 more
TL;DR: It is observed that CLU knockdown using the CLU inhibitor OGX-011 significantly suppressed HCC metastasis in two metastatic models through inhibiting EIF3I/Akt/MMP13 signaling.
Journal ArticleDOI
Alternative approaches to Hsp90 modulation for the treatment of cancer
TL;DR: Current Hsp90 inhibitors, the chaperone cycle, and regulation of this cycle will be discussed.
Journal ArticleDOI
Gambogic acid identifies an isoform-specific druggable pocket in the middle domain of Hsp90β.
Kendrick Yim,Thomas Prince,Shiwei Qu,Fang Bai,Patricia A. Jennings,José N. Onuchic,Emmanuel A. Theodorakis,Leonard M. Neckers +7 more
TL;DR: GBA, a pharmacophore contained within the natural product gambogic acid that binds uniquely to a site in Hsp90β, is identified as a prototype of a new class of isoform-specific Hsp 90 inhibitors, providing a new chemical tool to study the unique biological role of this abundantly expressed molecular chaperone in health and disease.
References
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Journal ArticleDOI
HSP90 and the chaperoning of cancer.
TL;DR: Pharmacologically 'bribing' the essential guard duty of the chaperone HSP90 (heat-shock protein of 90 kDa) seems to offer a unique anticancer strategy of considerable promise.
Journal ArticleDOI
Inhibition of heat shock protein HSP90-pp60v-src heteroprotein complex formation by benzoquinone ansamycins: essential role for stress proteins in oncogenic transformation.
TL;DR: It is demonstrated that HSP participation in multimolecular complex formation is required for src-mediated transformation and can provide a target for drug modulation.
Journal ArticleDOI
A high-affinity conformation of Hsp90 confers tumour selectivity on Hsp90 inhibitors.
Adeela Kamal,Lia Thao,John Sensintaffar,Lin Zhang,Marcus F. Boehm,Lawrence C. Fritz,Francis Burrows +6 more
TL;DR: In this article, the authors reported that Hsp90 derived from tumour cells has a 100-fold higher binding affinity for 17-AAG than does Hsp 90 from normal cells.
Journal Article
A high-affinity conformation of Hsp90 confers tumor selectivity on Hsp90 inhibitors
Adeela Kamal,John Sensintaffar,Patricia Karjian,Lin Zhang,Marcus F. Boehm,Lawrence C. Fritz,Francis Burrows +6 more
TL;DR: The results suggest that tumour cells contain Hsp90 complexes in an activated, high-affinity conformation that facilitates malignant progression, and that may represent a unique target for cancer therapeutics.
Journal ArticleDOI
The co-chaperone CHIP regulates protein triage decisions mediated by heat-shock proteins.
Patrice Connell,Carol A. Ballinger,Jihong Jiang,Yaxu Wu,Larry J. Thompson,Jörg Höhfeld,Jörg Höhfeld,Cam Patterson +7 more
TL;DR: It is shown that CHIP abolishes the steroid-binding activity and transactivation potential of the glucocorticoid receptor, a well-characterized Hsp90 substrate, even though it has little effect on its synthesis.