Cancer cell responses to Hsp70 inhibitor JG-98: Comparison with Hsp90 inhibitors and finding synergistic drug combinations

Yaglom, Julia A.; Wang, Yongmei; Li, Amy; Li, Zhenghu; Monti, Stefano; Alexandrov, Ilya; Lu, Xiongbin; Sherman, Michael Y.

doi:10.1038/s41598-017-14900-0

Cited by 51 publications

(60 citation statements)

References 43 publications

(48 reference statements)

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“…Interesting results were gained by Li and colleagues with JG-98 inhibitor. JG-98 disrupts HSP70-BAG3 complex, thereby, freezing HSP70 in its ADP state [213,214]. Similar effects were reported with YM-1, an inhibitor that targets HSP70-NEF complex, indicating that freezing of HSP70 in ADP-bound state can be the most promising strategy for the future developments of anti-cancer drugs [168].…”

Section: Small Molecule Inhibitors Of Hsp70 Cyclesupporting

confidence: 56%

HSP70 Multi-Functionality in Cancer

Albakova

Армеев

Kanevskiy

et al. 2020

Cells

176

141

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The 70-kDa heat shock proteins (HSP70s) are abundantly present in cancer, providing malignant cells selective advantage by suppressing multiple apoptotic pathways, regulating necrosis, bypassing cellular senescence program, interfering with tumor immunity, promoting angiogenesis and supporting metastasis. This direct involvement of HSP70 in most of the cancer hallmarks explains the phenomenon of cancer “addiction” to HSP70, tightly linking tumor survival and growth to the HSP70 expression. HSP70 operates in different states through its catalytic cycle, suggesting that it can multi-function in malignant cells in any of these states. Clinically, tumor cells intensively release HSP70 in extracellular microenvironment, resulting in diverse outcomes for patient survival. Given its clinical significance, small molecule inhibitors were developed to target different sites of the HSP70 machinery. Furthermore, several HSP70-based immunotherapy approaches were assessed in clinical trials. This review will explore different roles of HSP70 on cancer progression and emphasize the importance of understanding the flexibility of HSP70 nature for future development of anti-cancer therapies.

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Section: Small Molecule Inhibitors Of Hsp70 Cyclesupporting

confidence: 56%

HSP70 Multi-Functionality in Cancer

Albakova

Армеев

Kanevskiy

et al. 2020

Cells

176

141

View full text Add to dashboard Cite

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“…Furthermore, antiparallel dimeric Hsp70 species were detected in in vitro reconstituted complexes involving Hsp90, Hop, Hsp40, and GR (Glucocorticoid receptor) (27), supporting the functional role of Hsp70 dimerization in multichaperone assemblies. The level of inducible Hsp70 is elevated under proteotoxic conditions and chronically increased in some pathologies, including cancer (73)(74)(75)(76)(77)(78). Given that intracellular concentrations of Hsp70 can reach up to tens of M under stress conditions (79,80), the physiological importance of ATP-dependent Hsp70 dimers for overcoming proteotoxic stress becomes a likely hypothesis.…”

Section: Discussionmentioning

confidence: 99%

Human Stress-inducible Hsp70 Has a High Propensity to Form ATP-dependent Antiparallel Dimers That Are Differentially Regulated by Cochaperone Binding*

Trčka

Ďurech

Vaňková

et al. 2019

Molecular & Cellular Proteomics

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In BriefThe oligomerization (and particularly dimerization) of Hsp70 proteins plays an important role in their chaperoning activities.Here, we report that human stress-inducible Hsp70 possesses the highest propensity among analyzed Hsp70 homologs to form dimers in the presence of ATP. ATP-bound Hsp70 assembles in solution as an antiparallel dimer closely resembling the dimeric structures captured in DnaK and BiP crystals. ATP-dependent Hsp70 dimerization is necessary for efficient Hsp40 interaction and is differentially affected by TPR cochaperone binding. Graphical Abstract Highlights• Hsp70 homologs differ in their oligomeric properties in the presence of ATP.• Human inducible Hsp70 forms ATP-dependent anti-parallel dimers with high propensity.• Dimerization of ATP-bound Hsp70 is required for effective Hsp70-Hsp40 interaction.• ATP-dependent interaction with Tomm34 TPR cochaperone disrupts Hsp70 dimer.

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“…Therefore, based on a previous report (85), we sought to test a model in which the negative loop on ERK activity in mutant mice that depends on the DUSP6 phosphatase activity could involve a second level of regulation with critical direct participation of BAG3, a cochaperone of HSP70 and potent regulator and enhancer of DUSP6-ERK1/2 interaction. Notably, a well-defined HSP70-BAG3 interaction network has been described to act as a broadly acting regulator of cancer cell signaling factors (86,87). According to this finding, depletion of HSP70 not only is expected to increase ERK1/2-BAG3 interaction, which in turn suppresses p-ERK1/2 activity, but also could cause disruption of HSP70-BAG3 complexes, thus amplifying the antitumor effects.…”

Section: Loss Of Hsp70 Inhibits Den-induced Hcc Development By Triggementioning

confidence: 97%

The Molecular Chaperone Heat Shock Protein 70 Controls Liver Cancer Initiation and Progression by Regulating Adaptive DNA Damage and Mitogen-Activated Protein Kinase/Extracellular Signal-Regulated Kinase Signaling Pathways

et al. 2019

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Delineating the mechanisms that drive hepatic injury and hepatocellular carcinoma (HCC) progression is critical for development of novel treatments for recurrent and advanced HCC but also for the development of diagnostic and preventive strategies. Heat shock protein 70 (HSP70) acts in concert with several cochaperones and nucleotide exchange factors and plays an essential role in protein quality control that increases survival by protecting cells against environmental stressors. Specifically, the HSP70-mediated response has been implicated in the pathogenesis of cancer, but the specific mechanisms by which HSP70 may support malignant cell transformation remains to be fully elucidated. Here, we show that genetic ablation of HSP70 markedly impairs HCC initiation and progression by distinct but overlapping pathways. This includes the potentiation of the carcinogen-induced DNA damage response, at the tumor initiation stage, to increase the p53-dependent surveillance response leading to the cell cycle exit or death of genomically damaged differentiated pericentral hepatocytes, and this may also prevent their conversion into more proliferating HCC progenitor cells. Subsequently, activation of a mitogenactivated protein kinase/extracellular signal-regulated kinase (MAPK/ERK) negative feedback pathway diminishes oncogenic signals, thereby attenuating premalignant cell transformation and tumor progression. Modulation of HSP70 function may be a strategy for interfering with oncogenic signals driving liver cell transformation and tumor progression, thus providing an opportunity for human cancer control.

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Cancer cell responses to Hsp70 inhibitor JG-98: Comparison with Hsp90 inhibitors and finding synergistic drug combinations

Cited by 51 publications

References 43 publications

HSP70 Multi-Functionality in Cancer

HSP70 Multi-Functionality in Cancer

Human Stress-inducible Hsp70 Has a High Propensity to Form ATP-dependent Antiparallel Dimers That Are Differentially Regulated by Cochaperone Binding*

The Molecular Chaperone Heat Shock Protein 70 Controls Liver Cancer Initiation and Progression by Regulating Adaptive DNA Damage and Mitogen-Activated Protein Kinase/Extracellular Signal-Regulated Kinase Signaling Pathways

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