Sunitinib Dose Escalation Overcomes Transient Resistance in Clear Cell Renal Cell Carcinoma and Is Associated with Epigenetic Modifications

Adelaiye, Remi; Ciamporcero, Eric; Miles, Kiersten Marie; Sotomayor, Paula; Bard, Jonathan; Tsompana, Maria; Conroy, Dylan; Шен, Ли; Ramakrishnan, Swathi; Ku, Sheng-Yu; Orillion, Ashley; Prey, Joshua; Fetterly, Gerald J.; Buck, Michael; Chintala, Sreenivasulu; Bjarnason, Georg A.; Пили, Роберто

doi:10.1158/1535-7163.mct-14-0208

Cited by 62 publications

(71 citation statements)

References 32 publications

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“…This dual mechanism thus not only can contribute to resistance to sunitinib, but also can represent a mechanism by which higher doses of sunitinib exert cytotoxicity. Several reports have shown that cancer patients who resisted and subsequently progressed in response to clinically approved doses of sunitinib as well as during "sunitinib-off " period can be sensitized to sunitinib by escalating its dose (11,48). Our data shown here provide a potential molecular explanation for this reported observation, as higher doses of sunitinib could shift the response of tumor cells toward MCL-1 destabilization and mTOR inhibition, with an increased anticancer effect.…”

Section: Sunitinib Exerts Dual Effects On Mcl-1 and Mtor In Tolerant Andsupporting

confidence: 56%

“…Sunitinib is approved for treating patients with advanced renal cell carcinoma (2), pancreatic neuroendocrine tumors (3), and gastrointestinal stromal tumors (4,5) and is being tested in other types of cancer including osteosarcoma (6), colorectal cancer (7), and melanoma (8). However, a substantial percentage of patients are intrinsically resistant to sunitinib, and most patients who show initial response to treatment with sunitinib eventually relapse and develop progressive disease secondary to acquired sunitinib resistance, resulting in a modest overall therapeutic benefit (9)(10)(11)(12)(13). Optimal clinical use of sunitinib therefore relies on better understanding of the mechanisms of tumor resistance to this anticancer agent.…”

Section: Introductionmentioning

confidence: 99%

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Dual modulation of MCL-1 and mTOR determines the response to sunitinib

Elgendy

Abdel-Aziz

Renne

et al. 2016

Journal of Clinical Investigation

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Section: Sunitinib Exerts Dual Effects On Mcl-1 and Mtor In Tolerant Andsupporting

confidence: 56%

Section: Introductionmentioning

confidence: 99%

Dual modulation of MCL-1 and mTOR determines the response to sunitinib

Elgendy

Abdel-Aziz

Renne

et al. 2016

Journal of Clinical Investigation

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“…This observation may at least in part explain better DFS benefit of sunitinib in S-TRAC, relative to that reported in the ASSURE trial. In consequence, dose escalations such as described by Bjarnason et al [11,12], might result in better DFS and possibly also in better OS and dose individualization may warrant consideration, if adjuvant sunitinib therapy is considered.…”

Section: Cuaj -Consensus Statementmentioning

confidence: 99%

Kidney Cancer Research Network of Canada (KCRNC) consensus statement on the role of adjuvant therapy after nephrectomy for high-risk, non-metastatic renal cell carcinoma: A comprehensive analysis of the literature and meta-analysis of randomized controlled trials

Karakiewicz

Zaffuto

Kapoor

et al. 2018

CUAJ

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Introduction: The Kidney Cancer Research Network of Canada (KCRNC) collaborated to prepare this consensus statement about the use of target agents as adjuvant therapy in patients with nonmetastatic renal cell carcinoma (nmRCC) after nephrectomy. We reviewed the published data and performed a meta-analysis of studies that focused on vascular endothelial growth factor receptor (VEGFR) tyrosine kinase inhibitors (TKIs).Methods: A systematic literature search identified seven trials on adjuvant target therapy in nmRCC. Three trials, the ASSURE, S-TRAC, and PROTECT, focused on VEGFR TKIs and represented the focus of the study, including a meta-analysis combining their data on disease-free survival (DFS) and overall survival (OS).Results: The ASSURE trial showed no DFS or OS benefit of TKIs over placebo after one year of adjuvant sorafenib or sunitinib. In contrast, the S-TRAC trial showed improved DFS after one year of adjuvant sunitinib using central review process, but not using investigator review process. No OS benefit was recorded in either study. Recently, the PROTECT trial also showed no DFS or OS benefit when one year of adjuvant pazopanib was compared to placebo. Meta-analyses of the pooled DFS and OS estimates from all three trials resulted in DFS and OS hazard ratios of 0.87 (95% confidence interval [CI] 0.73‒1.04) and 1.04 (95% CI 0.89‒1.22), respectively.Conclusions: Data from three available clinical trials of adjuvant VEGFR TKIs vs. placebo do not currently support the use of adjuvant TKI therapy as standard of care after nephrectomy for nmRCC. At this time, adjuvant TKI-based adjuvant therapy is not recommended for routine use after nephrectomy for high-risk nmRCC, but highly motivated patients may benefit from a discussion with their oncologist regarding the risks and benefits of adjuvant TKI.

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“…6 This may explain the clinical observation of reduced toxicity as patients stay on tyrosine kinase inhibitor (TKI) therapy. These observations led to our early attempts to individualize dose and schedule to toxicity, 7,8 assuming toxicity might correlate better with sunitinib pharmacodynamics (PD) 9 and would take into account the inter-individual differences in sunitinib PK, potential decline in PK over time, individual singlenucleotide polymorphisms, and interactions with other drugs and that can impact the PK for sunitinib.…”

Section: Maximizing Drug Exposure Is Importantmentioning

confidence: 99%