Literature DB >> 27267850

A Novel HSP90 Inhibitor-Drug Conjugate to SN38 Is Highly Effective in Small Cell Lung Cancer.

Anna V Gaponova1,2, Anna S Nikonova1, Alexander Deneka1,2, Meghan C Kopp1,3, Alexander E Kudinov4, Natalia Skobeleva1, Vladimir Khazak5, Luisa S Ogawa6, Kathy Q Cai1, Kelly E Duncan7, James S Duncan7, Brian L Egleston1, David A Proia6, Yanis Boumber4, Erica A Golemis1.   

Abstract

PURPOSE: Small cell lung cancer (SCLC) is a highly aggressive disease representing 12% to 13% of total lung cancers, with median survival of <2 years. No targeted therapies have proven effective in SCLC. Although most patients respond initially to cytotoxic chemotherapies, resistance rapidly emerges, response to second-line agents is limited, and dose-limiting toxicities (DLT) are a major issue. This study performs preclinical evaluation of a new compound, STA-8666, in SCLC. EXPERIMENTAL
DESIGN: To avoid DLT for useful cytotoxic agents, the recently developed drug STA-8666 combines a chemical moiety targeting active HSP90 (concentrated in tumors) fused via cleavable linker to SN38, the active metabolite of irinotecan. We compare potency and mechanism of action of STA-8666 and irinotecan in vitro and in vivo
RESULTS: In two SCLC xenograft and patient-derived xenograft models, STA-8666 was tolerated without side effects up to 150 mg/kg. At this dose, STA-8666 controlled or eliminated established tumors whether used in a first-line setting or in tumors that had progressed following treatment on standard first- and second-line agents for SCLC. At 50 mg/kg, STA-8666 strongly enhanced the action of carboplatin. Pharmacokinetic profiling confirmed durable STA-8666 exposure in tumors compared with irinotecan. STA-8666 induced a more rapid, robust, and stable induction of cell-cycle arrest, expression of signaling proteins associated with DNA damage and cell-cycle checkpoints, and apoptosis in vitro and in vivo, in comparison with irinotecan.
CONCLUSIONS: Together, these results strongly support clinical development of STA-8666 for use in the first- or second-line setting for SCLC. Clin Cancer Res; 22(20); 5120-9. ©2016 AACR. ©2016 American Association for Cancer Research.

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Year:  2016        PMID: 27267850      PMCID: PMC5065742          DOI: 10.1158/1078-0432.CCR-15-3068

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  23 in total

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7.  Treatment of small cell lung cancer in academic and community settings: factors associated with receiving standard therapy and survival.

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Authors:  C-H Lai; K-S Park; D-H Lee; A T Alberobello; M Raffeld; M Pierobon; E Pin; E F Petricoin Iii; Y Wang; G Giaccone
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2.  Tumor-targeted SN38 inhibits growth of early stage non-small cell lung cancer (NSCLC) in a KRas/p53 transgenic mouse model.

Authors:  Alexander Y Deneka; Leora Haber; Meghan C Kopp; Anna V Gaponova; Anna S Nikonova; Erica A Golemis
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3.  Targeted delivery of chemotherapy using HSP90 inhibitor drug conjugates is highly active against pancreatic cancer models.

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Journal:  Oncotarget       Date:  2017-01-17

Review 4.  Tumor-Targeted Drug Conjugates as an Emerging Novel Therapeutic Approach in Small Cell Lung Cancer (SCLC).

Authors:  Alexander Y Deneka; Yanis Boumber; Tim Beck; Erica A Golemis
Journal:  Cancers (Basel)       Date:  2019-09-03       Impact factor: 6.639

Review 5.  Topoisomerases and cancer chemotherapy: recent advances and unanswered questions.

Authors:  Mary-Ann Bjornsti; Scott H Kaufmann
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6.  Evaluation of the Small-molecule BRD4 Degrader CFT-2718 in Small-cell Lung Cancer and Pancreatic Cancer Models.

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Journal:  Mol Cancer Ther       Date:  2021-05-27       Impact factor: 6.261

7.  STA-8666, a novel HSP90 inhibitor/SN-38 drug conjugate, causes complete tumor regression in preclinical mouse models of pediatric sarcoma.

Authors:  Christine M Heske; Arnulfo Mendoza; Leah D Edessa; Joshua T Baumgart; Sunmin Lee; Jane Trepel; David A Proia; Len Neckers; Lee J Helman
Journal:  Oncotarget       Date:  2016-10-04
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