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1. Multifaceted intervention by the Hsp90 inhibitor ganetespib (STA-9090) in cancer cells with activated JAK/STAT signaling.

Author

David A Proia, Kevin P Foley, Tim Korbut, Jim Sang, Don Smith, Richard C Bates, Yuan Liu, Alex F Rosenberg, Dan Zhou, Keizo Koya, James Barsoum, and Ronald K Blackman

Subjects
Medicine, Science
Abstract

There is accumulating evidence that dysregulated JAK signaling occurs in a wide variety of cancer types. In particular, mutations in JAK2 can result in the constitutive activation of STAT transcription factors and lead to oncogenic growth. JAK kinases are established Hsp90 client proteins and here we show that the novel small molecule Hsp90 inhibitor ganetespib (formerly STA-9090) exhibits potent in vitro and in vivo activity in a range of solid and hematological tumor cells that are dependent on JAK2 activity for growth and survival. Of note, ganetespib treatment results in sustained depletion of JAK2, including the constitutively active JAK2(V617F) mutant, with subsequent loss of STAT activity and reduced STAT-target gene expression. In contrast, treatment with the pan-JAK inhibitor P6 results in only transient effects on these processes. Further differentiating these modes of intervention, RNA and protein expression studies show that ganetespib additionally modulates cell cycle regulatory proteins, while P6 does not. The concomitant impact of ganetespib on both cell growth and cell division signaling translates to potent antitumor efficacy in mouse models of xenografts and disseminated JAK/STAT-driven leukemia. Overall, our findings support Hsp90 inhibition as a novel therapeutic approach for combating diseases dependent on JAK/STAT signaling, with the multimodal action of ganetespib demonstrating advantages over JAK-specific inhibitors.

Published
2011
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2. Data from mTOR Inhibition Potentiates HSP90 Inhibitor Activity via Cessation of HSP Synthesis

Author

David A. Proia, Richard C. Bates, Chaohua Zhang, Manuel Sequeira, Donald L. Smith, Jim Sang, Suqin He, and Jaime Acquaviva

Abstract

Because of their pleiotropic effects on critical oncoproteins, inhibitors of HSP90 represent a promising new class of therapeutic agents for the treatment of human cancer. However, pharmacologic inactivation of HSP90 subsequently triggers a heat shock response that may mitigate the full therapeutic benefit of these compounds. To overcome this limitation, a clinically feasible method was sought to block HSP synthesis induced by the potent HSP90 inhibitor ganetespib. An immunoassay screen of 322 late-stage or clinically approved drugs was performed to uncover compounds that could block upregulation of the stress-inducible HSP70 that results as a consequence of HSP90 blockade. Interestingly, inhibitors of the phosphoinositide 3-kinase (PI3K)/mTOR class counteracted ganetespib-induced HSP70 upregulation at both the gene and protein level by suppressing nuclear translocation of heat shock factor 1 (HSF1), the dominant transcription factor controlling cellular stress responses. This effect was conserved across multiple tumor types and was found to be regulated, in part, by mTOR-dependent translational activity. Pretreatment with cycloheximide, PI3K/mTOR inhibitor, or an inhibitor of eIF4E (a translation initiation factor and downstream effector of mTOR) all reduced ganetespib-mediated nuclear HSF1 accumulation, indicating that mTOR blockade confers a negative regulatory effect on HSF1 activity. Moreover, combined therapy regimens with mTOR or dual PI3K/mTOR inhibitors potentiated the antitumor efficacy of ganetespib in multiple in vivo models.Implications: Collectively these data identify a novel strategy to optimize the therapeutic potential of HSP90 inhibitors. Mol Cancer Res; 12(5); 703–13. ©2014 AACR.

Published
2023

5. Data from HSP90 Inhibitor–SN-38 Conjugate Strategy for Targeted Delivery of Topoisomerase I Inhibitor to Tumors

Author

Weiwen Ying, Dinesh Chimmanamada, Richard C. Bates, Sami Osman, Noriaki Tatsuta, Takayo Inoue, Igor Astsaturov, Vladimir Khazak, Chaohua Zhang, Suqin He, Jaime Acquaviva, Manuel Sequeira, Luisa Shin Ogawa, Jim Sang, John-Paul Jimenez, Junyi Zhang, Donald L. Smith, and David A. Proia

Abstract

The clinical benefits of chemotherapy are commonly offset by insufficient drug exposures, narrow safety margins, and/or systemic toxicities. Over recent decades, a number of conjugate-based targeting approaches designed to overcome these limitations have been explored. Here, we report on an innovative strategy that utilizes HSP90 inhibitor–drug conjugates (HDC) for directed tumor targeting of chemotherapeutic agents. STA-12-8666 is an HDC that comprises an HSP90 inhibitor fused to SN-38, the active metabolite of irinotecan. Mechanistic analyses in vitro established that high-affinity HSP90 binding conferred by the inhibitor backbone could be exploited for conjugate accumulation within tumor cells. In vivo modeling showed that the HSP90 inhibitor moiety was required for selective retention of STA-12-8666, and this enrichment promoted extended release of active SN-38 within the tumor compartment. Indeed, controlled intratumoral payload release by STA-12-8666 contributed to a broad therapeutic window, sustained biomarker activity, and remarkable degree of efficacy and durability of response in multiple cell line and patient-derived xenograft models. Overall, STA-12-8666 has been developed as a unique HDC agent that employs a distinct mechanism of targeted drug delivery to achieve potent and sustained antitumor effects. These findings identify STA-12-8666 as a promising new candidate for evaluation as novel anticancer therapeutic. Mol Cancer Ther; 14(11); 2422–32. ©2015 AACR.

Published
2023

6. Figure S1 from HSP90 Inhibitor–SN-38 Conjugate Strategy for Targeted Delivery of Topoisomerase I Inhibitor to Tumors

Author

Weiwen Ying, Dinesh Chimmanamada, Richard C. Bates, Sami Osman, Noriaki Tatsuta, Takayo Inoue, Igor Astsaturov, Vladimir Khazak, Chaohua Zhang, Suqin He, Jaime Acquaviva, Manuel Sequeira, Luisa Shin Ogawa, Jim Sang, John-Paul Jimenez, Junyi Zhang, Donald L. Smith, and David A. Proia

Abstract

HSP90 binding promotes the intracellular retention of HSP90 inhibitor-BODIPY probes in tumor cell lines.

Published
2023

8. Data from Targeting KRAS-Mutant Non–Small Cell Lung Cancer with the Hsp90 Inhibitor Ganetespib

Author

David A. Proia, Yumiko Wada, Chaohua Zhang, Manuel Sequeira, Suqin He, Julie C. Friedland, Jim Sang, Donald L. Smith, and Jaime Acquaviva

Abstract

Mutant KRAS is a feature of more than 25% of non–small cell lung cancers (NSCLC) and represents one of the most prevalent oncogenic drivers in this disease. NSCLC tumors with oncogenic KRAS respond poorly to current therapies, necessitating the pursuit of new treatment strategies. Targeted inhibition of the molecular chaperone Hsp90 results in the coordinated blockade of multiple oncogenic signaling pathways in tumor cells and has thus emerged as an attractive avenue for therapeutic intervention in human malignancies. Here, we examined the activity of ganetespib, a small-molecule inhibitor of Hsp90 currently in clinical trials for NSCLCs in a panel of lung cancer cell lines harboring a diverse spectrum of KRAS mutations. In vitro, ganetespib was potently cytotoxic in all lines, with concomitant destabilization of KRAS signaling effectors. Combinations of low-dose ganetespib with MEK or PI3K/mTOR inhibitors resulted in superior cytotoxic activity than single agents alone in a subset of mutant KRAS cells, and the antitumor efficacy of ganetespib was potentiated by cotreatment with the PI3K/mTOR inhibitor BEZ235 in A549 xenografts in vivo. At the molecular level, ganetespib suppressed activating feedback signaling loops that occurred in response to MEK and PI3K/mTOR inhibition, although this activity was not the sole determinant of combinatorial benefit. In addition, ganetespib sensitized mutant KRAS NSCLC cells to standard-of-care chemotherapeutics of the antimitotic, topoisomerase inhibitor, and alkylating agent classes. Taken together, these data underscore the promise of ganetespib as a single-agent or combination treatment in KRAS-driven lung tumors. Mol Cancer Ther; 11(12); 2633–43. ©2012 AACR.

Published
2023

9. Table S1 from HSP90 Inhibitor–SN-38 Conjugate Strategy for Targeted Delivery of Topoisomerase I Inhibitor to Tumors

Author

Weiwen Ying, Dinesh Chimmanamada, Richard C. Bates, Sami Osman, Noriaki Tatsuta, Takayo Inoue, Igor Astsaturov, Vladimir Khazak, Chaohua Zhang, Suqin He, Jaime Acquaviva, Manuel Sequeira, Luisa Shin Ogawa, Jim Sang, John-Paul Jimenez, Junyi Zhang, Donald L. Smith, and David A. Proia

Abstract

Cross-species plasma stability of STA-12-8666 as a function of time

Published
2023

12. Data from Ganetespib, a Unique Triazolone-Containing Hsp90 Inhibitor, Exhibits Potent Antitumor Activity and a Superior Safety Profile for Cancer Therapy

Author

Keizo Koya, James Barsoum, Yumiko Wada, Luisa Shin Ogawa, Jamie Acquaviva, Shuxia Ye, Jim Sang, Noriaki Tatsuta, Takayo Inoue, Dan Zhou, Ronald K. Blackman, David A. Proia, Kevin P. Foley, Lijun Sun, Zhenjian Du, and Weiwen Ying

Abstract

Targeted inhibition of the molecular chaperone Hsp90 results in the simultaneous blockade of multiple oncogenic signaling pathways and has, thus, emerged as an attractive strategy for the development of novel cancer therapeutics. Ganetespib (formerly known as STA-9090) is a unique resorcinolic triazolone inhibitor of Hsp90 that is currently in clinical trials for a number of human cancers. In the present study, we showed that ganetespib exhibits potent in vitro cytotoxicity in a range of solid and hematologic tumor cell lines, including those that express mutated kinases that confer resistance to small-molecule tyrosine kinase inhibitors. Ganetespib treatment rapidly induced the degradation of known Hsp90 client proteins, displayed superior potency to the ansamycin inhibitor 17-allylamino-17-demethoxygeldanamycin (17-AAG), and exhibited sustained activity even with short exposure times. In vivo, ganetespib showed potent antitumor efficacy in solid and hematologic xenograft models of oncogene addiction, as evidenced by significant growth inhibition and/or regressions. Notably, evaluation of the microregional activity of ganetespib in tumor xenografts showed that ganetespib was efficiently distributed throughout tumor tissue, including hypoxic regions >150 μm from the microvasculature, to inhibit proliferation and induce apoptosis. Importantly, ganetespib showed no evidence of cardiac or liver toxicity. Taken together, this preclinical activity profile indicates that ganetespib may have broad application for a variety of human malignancies, and with select mechanistic and safety advantages over other first- and second-generation Hsp90 inhibitors. Mol Cancer Ther; 11(2); 475–84. ©2011 AACR.

Published
2023

17. Supplementary Table 1 from FGFR3 Translocations in Bladder Cancer: Differential Sensitivity to HSP90 Inhibition Based on Drug Metabolism

Author

David A. Proia, Richard C. Bates, Margaret A. Knowles, Noriaki Tatsuta, Takayo Inoue, Luisa Shin Ogawa, Donald L. Smith, Manuel Sequeira, Jim Sang, Masazumi Nagai, John-Paul Jimenez, Chaohua Zhang, Suqin He, and Jaime Acquaviva

Abstract

PDF - 67K, FGFR3 fusion-positive bladder cell line sensitivity and metabolism profiles of targeted anticancer compounds.

Published
2023

21. Data from Overcoming Acquired BRAF Inhibitor Resistance in Melanoma via Targeted Inhibition of Hsp90 with Ganetespib

Author

David A. Proia, Richard C. Bates, Jim Sang, Suqin He, Manuel Sequeira, Chaohua Zhang, John-Paul Jimenez, Donald L. Smith, and Jaime Acquaviva

Abstract

Activating BRAF kinase mutations serve as oncogenic drivers in over half of all melanomas, a feature that has been exploited in the development of new molecularly targeted approaches to treat this disease. Selective BRAFV600E inhibitors, such as vemurafenib, typically induce initial, profound tumor regressions within this group of patients; however, durable responses have been hampered by the emergence of drug resistance. Here, we examined the activity of ganetespib, a small-molecule inhibitor of Hsp90, in melanoma lines harboring the BRAFV600E mutation. Ganetespib exposure resulted in the loss of mutant BRAF expression and depletion of mitogen-activated protein kinase and AKT signaling, resulting in greater in vitro potency and antitumor efficacy compared with targeted BRAF and MAP–ERK kinase (MEK) inhibitors. Dual targeting of Hsp90 and BRAFV600E provided combinatorial benefit in vemurafenib-sensitive melanoma cells in vitro and in vivo. Importantly, ganetespib overcame mechanisms of intrinsic and acquired resistance to vemurafenib, the latter of which was characterized by reactivation of extracellular signal-regulated kinase (ERK) signaling. Continued suppression of BRAFV600E by vemurafenib potentiated sensitivity to MEK inhibitors after acquired resistance had been established. Ganetespib treatment reduced, but not abolished, elevations in steady-state ERK activity. Profiling studies revealed that the addition of a MEK inhibitor could completely abrogate ERK reactivation in the resistant phenotype, with ganetespib displaying superior combinatorial activity over vemurafenib. Moreover, ganetespib plus the MEK inhibitor TAK-733 induced tumor regressions in vemurafenib-resistant xenografts. Overall these data highlight the potential of ganetespib as a single-agent or combination treatment in BRAFV600E-driven melanoma, particularly as a strategy to overcome acquired resistance to selective BRAF inhibitors. Mol Cancer Ther; 13(2); 353–63. ©2014 AACR.

Published
2023

22. Supplementary Figure 1 from Targeted Inhibition of the Molecular Chaperone Hsp90 Overcomes ALK Inhibitor Resistance in Non–Small Cell Lung Cancer

Author

David A. Proia, Iman El-Hariry, Stephan W. Morris, D. Ross Camidge, Richard C. Bates, Suqin He, Robert C. Doebele, Alice T. Shaw, John-Paul Jimenez, Christine M. Lovly, Liquan Xue, Qin Jiang, Chaohua Zhang, Manuel Sequeira, Donald L. Smith, Julie C. Friedland, Jaime Acquaviva, and Jim Sang

Abstract

PDF file - 251K, Chemical structures of ganetespib and crizotinib.

Published
2023

23. Supplementary Figure 1 from FGFR3 Translocations in Bladder Cancer: Differential Sensitivity to HSP90 Inhibition Based on Drug Metabolism

Author

David A. Proia, Richard C. Bates, Margaret A. Knowles, Noriaki Tatsuta, Takayo Inoue, Luisa Shin Ogawa, Donald L. Smith, Manuel Sequeira, Jim Sang, Masazumi Nagai, John-Paul Jimenez, Chaohua Zhang, Suqin He, and Jaime Acquaviva

Abstract

PDF - 667K, Ganetespib treatment overcomes the FGFR inhibitor resistant phenotype in FGFR3 mutant bladder cancer cell lines.

Published
2023

25. Data from FGFR3 Translocations in Bladder Cancer: Differential Sensitivity to HSP90 Inhibition Based on Drug Metabolism

Author

David A. Proia, Richard C. Bates, Margaret A. Knowles, Noriaki Tatsuta, Takayo Inoue, Luisa Shin Ogawa, Donald L. Smith, Manuel Sequeira, Jim Sang, Masazumi Nagai, John-Paul Jimenez, Chaohua Zhang, Suqin He, and Jaime Acquaviva

Abstract

Activating mutations and/or overexpression of FGFR3 are common in bladder cancer, making FGFR3 an attractive therapeutic target in this disease. In addition, FGFR3 gene rearrangements have recently been described that define a unique subset of bladder tumors. Here, a selective HSP90 inhibitor, ganetespib, induced loss of FGFR3-TACC3 fusion protein expression and depletion of multiple oncogenic signaling proteins in RT112 bladder cells, resulting in potent cytotoxicity comparable with the pan-FGFR tyrosine kinase inhibitor BGJ398. However, in contrast to BGJ398, ganetespib exerted pleiotropic effects on additional mitogenic and survival pathways and could overcome the FGFR inhibitor–resistant phenotype of FGFR3 mutant–expressing 97-7 and MHG-U3 cells. Combinatorial benefit was observed when ganetespib was used with BGJ398 both in vitro and in vivo. Interestingly, two additional FGFR3 fusion-positive lines (RT4 and SW480) retained sensitivity to HSP90 inhibitor treatment by the ansamycins 17-AAG and 17-DMAG yet displayed intrinsic resistance to ganetespib or AUY922, both second-generation resorcinol-based compounds. Both cell lines, compared with RT112, expressed considerably higher levels of endogenous UGT1A enzyme; this phenotype resulted in a rapid glucuronidation-dependent metabolism and subsequent efflux of ganetespib from SW780 cells, thus providing a mechanism to account for the lack of bioactivity.Implications: Pharmacologic blockade of the molecular chaperone HSP90 represents a promising approach for treating bladder tumors driven by oncogenic gene rearrangements of FGFR3. Furthermore, UDP-glucuronosyltransferase enzyme expression may serve as a predictive factor for clinical response to resorcinol-based HSP90 inhibitors. Mol Cancer Res; 12(7); 1042–54. ©2014 AACR.

Published
2023

26. Supplementary Methods and Figure Legends from Targeted Inhibition of the Molecular Chaperone Hsp90 Overcomes ALK Inhibitor Resistance in Non–Small Cell Lung Cancer

Author

David A. Proia, Iman El-Hariry, Stephan W. Morris, D. Ross Camidge, Richard C. Bates, Suqin He, Robert C. Doebele, Alice T. Shaw, John-Paul Jimenez, Christine M. Lovly, Liquan Xue, Qin Jiang, Chaohua Zhang, Manuel Sequeira, Donald L. Smith, Julie C. Friedland, Jaime Acquaviva, and Jim Sang

Abstract

PDF file - 71K

Published
2023

27. Supplementary Figure 3 from Targeted Inhibition of the Molecular Chaperone Hsp90 Overcomes ALK Inhibitor Resistance in Non–Small Cell Lung Cancer

Author

David A. Proia, Iman El-Hariry, Stephan W. Morris, D. Ross Camidge, Richard C. Bates, Suqin He, Robert C. Doebele, Alice T. Shaw, John-Paul Jimenez, Christine M. Lovly, Liquan Xue, Qin Jiang, Chaohua Zhang, Manuel Sequeira, Donald L. Smith, Julie C. Friedland, Jaime Acquaviva, and Jim Sang

Abstract

PDF file - 486K, The addition of ganetespib to crizotinib does not result in added toxicity in H3122 xenografts.

Published
2023

30. Supplementary Figure 4 from Targeted Inhibition of the Molecular Chaperone Hsp90 Overcomes ALK Inhibitor Resistance in Non–Small Cell Lung Cancer

Author

David A. Proia, Iman El-Hariry, Stephan W. Morris, D. Ross Camidge, Richard C. Bates, Suqin He, Robert C. Doebele, Alice T. Shaw, John-Paul Jimenez, Christine M. Lovly, Liquan Xue, Qin Jiang, Chaohua Zhang, Manuel Sequeira, Donald L. Smith, Julie C. Friedland, Jaime Acquaviva, and Jim Sang

Abstract

PDF file - 2538K, Crizotinib-resistant H3122 CR1 cells express an EMT phenotype.

Published
2023

37. Supplementary Table 1 from Ganetespib (STA-9090), a Nongeldanamycin HSP90 Inhibitor, Has Potent Antitumor Activity in In Vitro and In Vivo Models of Non–Small Cell Lung Cancer

Author

Geoffrey I. Shapiro, Kwok-Kin Wong, James Barsoum, Weiwen Ying, Matthew Meyerson, John-Paul Jimenez, Christa L. Borgman, Christopher D. Carey, Papiya Sinha, Yu-Chen Li, Julian Carretero, Danan Li, Liang Chen, Takayo Inoue, Scott J. Rodig, Jim Sang, Kevin P. Foley, Samanthi A. Perera, and Takeshi Shimamura

Abstract

PDF file, 560K, Comparison of ganetespib and 17-AAG efficacy in NSCLC cell lines.

Published
2023

38. Data from Preclinical Activity Profile and Therapeutic Efficacy of the HSP90 Inhibitor Ganetespib in Triple-Negative Breast Cancer

Author

Iman El-Hariry, Richard C. Bates, Jim Sang, Donald L. Smith, Jaime Acquaviva, Masazumi Nagai, Sara Tolaney, Geoffrey I. Shapiro, Neil Spector, Suqin He, John-Paul Jimenez, Manuel Sequeira, Chaohua Zhang, and David A. Proia

Abstract

Purpose: Treatment options for patients with triple-negative breast cancer (TNBC) are largely limited to systemic chemotherapies, which have shown disappointing efficacy in the metastatic setting. Here, we undertook a comprehensive evaluation of the activity of ganetespib, a potent inhibitor of HSP90, in this malignancy.Experimental Design: The antitumor and antimetastatic activity of ganetespib was investigated using TNBC cell lines and xenograft models. Combinatorial drug analyses were performed with chemotherapeutic agents and concomitant effects on DNA damage and cell-cycle disruption were assessed in vitro; antitumor efficacy was assessed in vivo. Metabolic and objective tumor responses were evaluated in patients with metastatic TNBC undergoing ganetespib treatment.Results: Ganetespib simultaneously deactivated multiple oncogenic pathways to potently reduce cell viability in TNBC cell lines, and suppressed lung metastases in experimental models. Ganetespib potentiated the cytotoxic activity of doxorubicin via enhanced DNA damage and mitotic arrest, conferring superior efficacy to the doxorubicin–cyclophosphamide regimen in TNBC xenografts. Ganetespib also promoted mitotic catastrophe and apoptosis in combination with taxanes in vitro, and these effects translated to significantly improved combinatorial activity in vivo. Marked tumor shrinkage of metastatic lung and lymphatic lesions were seen in patients on ganetespib monotherapy.Conclusion: The preclinical activity profile and clinical evidence of tumor regression suggest that ganetespib offers considerable promise as a new therapeutic candidate to target TNBC. Clin Cancer Res; 20(2); 413–24. ©2013 AACR.

Published
2023

39. Data from Ganetespib (STA-9090), a Nongeldanamycin HSP90 Inhibitor, Has Potent Antitumor Activity in In Vitro and In Vivo Models of Non–Small Cell Lung Cancer

Author

Geoffrey I. Shapiro, Kwok-Kin Wong, James Barsoum, Weiwen Ying, Matthew Meyerson, John-Paul Jimenez, Christa L. Borgman, Christopher D. Carey, Papiya Sinha, Yu-Chen Li, Julian Carretero, Danan Li, Liang Chen, Takayo Inoue, Scott J. Rodig, Jim Sang, Kevin P. Foley, Samanthi A. Perera, and Takeshi Shimamura

Abstract

Purpose: We describe the anticancer activity of ganetespib, a novel non-geldanamycin heat shock protein 90 (HSP90) inhibitor, in non-small cell lung cancer (NSCLC) models.Experimental Design: The activity of ganetespib was compared with that of the geldanamycin 17-AAG in biochemical assays, cell lines, and xenografts, and evaluated in an ERBB2 YVMA-driven mouse lung adenocarcinoma model.Results: Ganetespib blocked the ability of HSP90 to bind to biotinylated geldanamycin and disrupted the association of HSP90 with its cochaperone, p23, more potently than 17-AAG. In genomically defined NSCLC cell lines, ganetespib caused depletion of receptor tyrosine kinases, extinguishing of downstream signaling, inhibition of proliferation and induction of apoptosis with IC50 values ranging 2 to 30 nmol/L, substantially lower than those required for 17-AAG (20–3,500 nmol/L). Ganetespib was also approximately 20-fold more potent in isogenic Ba/F3 pro-B cells rendered IL-3 independent by expression of EGFR and ERBB2 mutants. In mice bearing NCI-H1975 (EGFR L858R/T790M) xenografts, ganetespib was rapidly eliminated from plasma and normal tissues but was maintained in tumor with t1/2 58.3 hours, supporting once-weekly dosing experiments, in which ganetespib produced greater tumor growth inhibition than 17-AAG. However, after a single dose, reexpression of mutant EGFR occurred by 72 hours, correlating with reversal of antiproliferative and proapoptotic effects. Consecutive day dosing resulted in xenograft regressions, accompanied by more sustained pharmacodynamic effects. Ganetespib also showed activity against mouse lung adenocarcinomas driven by oncogenic ERBB2 YVMA.Conclusions: Ganetespib has greater potency than 17-AAG and potential efficacy against several NSCLC subsets, including those harboring EGFR or ERBB2 mutation. Clin Cancer Res; 18(18); 4973–85. ©2012 AACR.

Published
2023

40. Supplementary Figure 2 from Preclinical Activity Profile and Therapeutic Efficacy of the HSP90 Inhibitor Ganetespib in Triple-Negative Breast Cancer

Author

Iman El-Hariry, Richard C. Bates, Jim Sang, Donald L. Smith, Jaime Acquaviva, Masazumi Nagai, Sara Tolaney, Geoffrey I. Shapiro, Neil Spector, Suqin He, John-Paul Jimenez, Manuel Sequeira, Chaohua Zhang, and David A. Proia

Abstract

PDF file - 2670K, Ganetespib treatment reduces lung metastatic burden in an experimental metastasis model and has minimal effects on primary tumor growth in an orthotopic model.

Published
2023

41. Supplementary Figure 1 from Ganetespib (STA-9090), a Nongeldanamycin HSP90 Inhibitor, Has Potent Antitumor Activity in In Vitro and In Vivo Models of Non–Small Cell Lung Cancer

Author

Geoffrey I. Shapiro, Kwok-Kin Wong, James Barsoum, Weiwen Ying, Matthew Meyerson, John-Paul Jimenez, Christa L. Borgman, Christopher D. Carey, Papiya Sinha, Yu-Chen Li, Julian Carretero, Danan Li, Liang Chen, Takayo Inoue, Scott J. Rodig, Jim Sang, Kevin P. Foley, Samanthi A. Perera, and Takeshi Shimamura

Abstract

PDF file, 1349K, Depletion of receptor tyrosine kinases and suppression of downstream signaling in HCC827 cells in response to 17-AAG or ganetespib-mediated HSP90 inhibition.

Published
2023

42. Supplementary Figure 3 from Ganetespib (STA-9090), a Nongeldanamycin HSP90 Inhibitor, Has Potent Antitumor Activity in In Vitro and In Vivo Models of Non–Small Cell Lung Cancer

Author

Geoffrey I. Shapiro, Kwok-Kin Wong, James Barsoum, Weiwen Ying, Matthew Meyerson, John-Paul Jimenez, Christa L. Borgman, Christopher D. Carey, Papiya Sinha, Yu-Chen Li, Julian Carretero, Danan Li, Liang Chen, Takayo Inoue, Scott J. Rodig, Jim Sang, Kevin P. Foley, Samanthi A. Perera, and Takeshi Shimamura

Abstract

PDF file, 365K, Activity of ganetespib in HCC827 xenografts.

Published
2023

43. Supplementary Figure 4 from Preclinical Activity Profile and Therapeutic Efficacy of the HSP90 Inhibitor Ganetespib in Triple-Negative Breast Cancer

Author

Iman El-Hariry, Richard C. Bates, Jim Sang, Donald L. Smith, Jaime Acquaviva, Masazumi Nagai, Sara Tolaney, Geoffrey I. Shapiro, Neil Spector, Suqin He, John-Paul Jimenez, Manuel Sequeira, Chaohua Zhang, and David A. Proia

Abstract

PDF file - 644K, Gantespib potentiates the efficacy of the microtubule dynamics inhibitor eribulin in TNBC xenografts.

Published
2023

44. Supplementary Figure 6 from Ganetespib (STA-9090), a Nongeldanamycin HSP90 Inhibitor, Has Potent Antitumor Activity in In Vitro and In Vivo Models of Non–Small Cell Lung Cancer

Author

Geoffrey I. Shapiro, Kwok-Kin Wong, James Barsoum, Weiwen Ying, Matthew Meyerson, John-Paul Jimenez, Christa L. Borgman, Christopher D. Carey, Papiya Sinha, Yu-Chen Li, Julian Carretero, Danan Li, Liang Chen, Takayo Inoue, Scott J. Rodig, Jim Sang, Kevin P. Foley, Samanthi A. Perera, and Takeshi Shimamura

Abstract

PDF file, 776K, Effects of 17-AAG and ganetespib on cell viability and mutant ERBB2 expression in ERBB2-dependent Ba/F3 cells.

Published
2023

45. Supplementary Table 2 from Ganetespib (STA-9090), a Nongeldanamycin HSP90 Inhibitor, Has Potent Antitumor Activity in In Vitro and In Vivo Models of Non–Small Cell Lung Cancer

Author

Geoffrey I. Shapiro, Kwok-Kin Wong, James Barsoum, Weiwen Ying, Matthew Meyerson, John-Paul Jimenez, Christa L. Borgman, Christopher D. Carey, Papiya Sinha, Yu-Chen Li, Julian Carretero, Danan Li, Liang Chen, Takayo Inoue, Scott J. Rodig, Jim Sang, Kevin P. Foley, Samanthi A. Perera, and Takeshi Shimamura

Abstract

PDF file, 136K, Median IC50's for NSCLC cell lines (with ganetespib and 17-AAG) with different genotypic subtypes.

Published
2023

46. Supplementary Table 3 from Ganetespib (STA-9090), a Nongeldanamycin HSP90 Inhibitor, Has Potent Antitumor Activity in In Vitro and In Vivo Models of Non–Small Cell Lung Cancer

Author

Geoffrey I. Shapiro, Kwok-Kin Wong, James Barsoum, Weiwen Ying, Matthew Meyerson, John-Paul Jimenez, Christa L. Borgman, Christopher D. Carey, Papiya Sinha, Yu-Chen Li, Julian Carretero, Danan Li, Liang Chen, Takayo Inoue, Scott J. Rodig, Jim Sang, Kevin P. Foley, Samanthi A. Perera, and Takeshi Shimamura

Abstract

PDF file, 361K, Comparison of EGFR TKI and HSP90 inhibitor efficacy in Ba/F3 cells ectopically expressing different EGFR mutations.

Published
2023

49. Supplementary Figure 2 from Ganetespib (STA-9090), a Nongeldanamycin HSP90 Inhibitor, Has Potent Antitumor Activity in In Vitro and In Vivo Models of Non–Small Cell Lung Cancer

Author

Geoffrey I. Shapiro, Kwok-Kin Wong, James Barsoum, Weiwen Ying, Matthew Meyerson, John-Paul Jimenez, Christa L. Borgman, Christopher D. Carey, Papiya Sinha, Yu-Chen Li, Julian Carretero, Danan Li, Liang Chen, Takayo Inoue, Scott J. Rodig, Jim Sang, Kevin P. Foley, Samanthi A. Perera, and Takeshi Shimamura

Abstract

PDF file, 1170K, Depletion of oncogenic drivers in NSCLC cell lines.

Published
2023

50. Supplementary Figure 4 from Ganetespib (STA-9090), a Nongeldanamycin HSP90 Inhibitor, Has Potent Antitumor Activity in In Vitro and In Vivo Models of Non–Small Cell Lung Cancer

Author

Geoffrey I. Shapiro, Kwok-Kin Wong, James Barsoum, Weiwen Ying, Matthew Meyerson, John-Paul Jimenez, Christa L. Borgman, Christopher D. Carey, Papiya Sinha, Yu-Chen Li, Julian Carretero, Danan Li, Liang Chen, Takayo Inoue, Scott J. Rodig, Jim Sang, Kevin P. Foley, Samanthi A. Perera, and Takeshi Shimamura

Abstract

PDF file, 719K, Comparison of once-weekly and consecutive day dosing schedules among individual mice bearing NCI-H1975 xenografts.

Published
2023

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