FGFR3 Translocations in Bladder Cancer: Differential Sensitivity to HSP90 Inhibition Based on Drug Metabolism

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

doi:10.1158/1541-7786.mcr-14-0004

Cited by 68 publications

(54 citation statements)

References 41 publications

(61 reference statements)

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“…The existence of FGFR3-TACC3 fusions in human cancers creates additional challenges and opportunities for identifying effective treatment strategies. For instance, a recent study showed that the HSP90 inhibitor ganetespib exerted pleiotropic effects on mitogenic and survival pathways in cells expressing oncogenic gene rearrangements of FGFR3, and provided an alternative therapeutic approach in addition to the pan-FGFR tyrosine kinase inhibitor BGJ398 (47). Further study of novel pathways activated by the FGFR3-TACC3 fusion protein, and a deeper understanding of the molecular details exploited by FGFR3-TACC3 to achieve its biologic potency, can be expected lead to novel therapeutic paradigms.…”

Section: Discussionmentioning

confidence: 99%

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Oncogenic Gene Fusion FGFR3-TACC3 Is Regulated by Tyrosine Phosphorylation

Nelson

Meyer

Siari

et al. 2016

Molecular Cancer Research

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Fibroblast growth factor receptors (FGFR) are critical for cell proliferation and differentiation. Mutation and/or translocation of FGFRs lead to aberrant signaling that often results in developmental syndromes or cancer growth. As sequencing of human tumors becomes more frequent, so does the detection of FGFR translocations and fusion proteins. The research conducted in this article examines a frequently identified fusion protein between FGFR3 and transforming acidic coiled-coil containing protein 3 (TACC3), frequently identified in glioblastoma, lung cancer, bladder cancer, oral cancer, head and neck squamous cell carcinoma, gallbladder cancer, and cervical cancer. Using titanium dioxide-based phosphopeptide enrichment (TiO 2 )-liquid chromatography (LC)-high mass accuracy tandem mass spectrometry (MS/MS), it was demonstrated that the fused coiled-coil TACC3 domain results in constitutive phosphorylation of key activating FGFR3 tyrosine residues. The presence of the TACC coiled-coil domain leads to increased and altered levels of FGFR3 activation, fusion protein phosphorylation, MAPK pathway activation, nuclear localization, cellular transformation, and IL3-independent proliferation. Introduction of K508R FGFR3 kinase-dead mutation abrogates these effects, except for nuclear localization which is due solely to the TACC3 domain.Implications: These results demonstrate that FGFR3 kinase activity is essential for the oncogenic effects of the FGFR3-TACC3 fusion protein and could serve as a therapeutic target, but that phosphorylated tyrosine residues within the TACC3-derived portion are not critical for activity.

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Section: Discussionmentioning

confidence: 99%

“…Received December 22, 2015; revised January 12, 2016; accepted February 3, 2016; published OnlineFirst February 11, 2016. …”

Section: Acknowledgmentsmentioning

confidence: 99%

Oncogenic Gene Fusion FGFR3-TACC3 Is Regulated by Tyrosine Phosphorylation

Nelson

Meyer

Siari

et al. 2016

Molecular Cancer Research

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“…insensitive to resorcinol-based HSP90 inhibitors due to endogenous glucoronidation (27). STA-12-8666 treatment significantly suppressed SW780 tumor growth (Fig.…”

Section: Hdc Exposure Is Therapeutically Superior To Combination Irinmentioning

confidence: 93%

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

Proia

Smith

Zhang

et al. 2015

Molecular Cancer Therapeutics

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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.

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“…Activation and dimerization of FGFR3 result in cell proliferation or differentiation via signal transduction pathways (10). Point mutations in transmembrane domain of FGFR3 have been identified as a causative factor for skeletal development disorders such as achondroplasia and hypochondroplasia (7,30).…”

Section: Discussionmentioning

confidence: 99%

“…Two membrane-proximal D2 and D3 domains, and interconnecting D2-D3 linker bear the determinants of ligand binding and specificity (10). The Ig-domain III is encoded by two separate exons, exon 8 and exon 9.…”

Section: Introductionmentioning

confidence: 99%

Phenotypic and Signaling Consequences of a Novel Aberrantly Spliced Transcript FGF Receptor-3 in Hepatocellular Carcinoma

Shen

Cheng

et al. 2016

Cancer Research

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Fibroblast growth factor receptor 3 (FGFR3) plays important roles in cell proliferation, differentiation, and angiogenesis. FGFR3 is abnormally upregulated in hepatocellular carcinoma (HCC), where it correlates positively with clinicopathologic index, HCC differentiation, and advanced nuclear grade. In this study, we describe an aberrantly spliced transcript of FGFR3, termed FGFR3 D7-9 , was identified as a high frequency even in HCC. FGFR3 D7-9 lacks exons encoding the immunoglobulin-like III domain and promoted the proliferation, migration, and metastasis of HCC cells both in vitro and in vivo. Coimmunoprecipation and surface plasmon resonance assays demonstrated that the binding affinity of the aberrant FGFR3 D7-9 receptor to FGFs was significantly higher than wild-type FGFR3 IIIc . Furthermore, FGFR3 D7-9 could be self-activated by homodimerization and autophosphorylation even in the absence of ligand. Finally, FGFR3 D7-9 more potently induced phosphorylation of the ERK and AKT kinases, leading to abnormal downstream signaling through the ERK and PI3K/AKT/mTOR pathways. FGFR3 D7-9 also upregulated the metastasis-associated molecules Snail, MMP-9, and downregulated E-cadherin, which associated directly with FGFR3 D7-9 . Thus, as a ligand-dependent or -independent receptor, FGFR3 D7-9 exerted multiple potent oncogenic functions in HCC cells, including proliferation, migration, and lung metastatic capacity. Overall, FGFR3 mRNA missplicing in HCC contributes significantly to its malignant character, with implications for therapeutic targeting. Cancer Res; 76(14); 4205-15. Ó2016 AACR.

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FGFR3 Translocations in Bladder Cancer: Differential Sensitivity to HSP90 Inhibition Based on Drug Metabolism

Cited by 68 publications

References 41 publications

Oncogenic Gene Fusion FGFR3-TACC3 Is Regulated by Tyrosine Phosphorylation

Oncogenic Gene Fusion FGFR3-TACC3 Is Regulated by Tyrosine Phosphorylation

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

Phenotypic and Signaling Consequences of a Novel Aberrantly Spliced Transcript FGF Receptor-3 in Hepatocellular Carcinoma

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