Genomic Biomarkers of a Randomized Trial Comparing First-line Everolimus and Sunitinib in Patients with Metastatic Renal Cell Carcinoma

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Genomic Biomarkers of a Randomized Trial Comparing First-line Everolimus and Sunitinib in Patients with Metastatic Renal Cell Carcinoma

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作者：James J. Hsieh^a ; ^{hsiehj@mskcc.org} ; David Chen^b ; Patricia I. Wang^a ; Mahtab Marker^b ; Almedina Redzematovic^a ; Ying-Bei Chen^a ; S. Duygu Selcuklu^a ; Nils Weinhold^a ; Nancy Bouvier^a ; Kety H. Huberman^a ; Umesh Bhanot^a ; Michael S. Chevinsky^a ; ^c ; Parul Patel^b ; Patrizia Pinciroli^a ; ^d ; Helen H. Won^a ; Daoqi You^a ; Agnes Viale^a ; William Lee^a ; A. Ari Hakimi^a ; Michael F. Berger^a ; Nicholas D. Socci^a ; Emily H. Cheng^a ; Jennifer Knox^e ; Martin H. Voss^a ; Maurizio Voi^b ; Robert J. Motzer^a
关键词：Genomic biomarker ; Kidney cancer ; Targeted therapy ; Everolimus ; Sunitinib ; Tumor suppressor gene ; PBRM1 ; SETD2 ; BAP1 ; KDM5C
刊名：European Urology
出版年：2017
出版时间：March 2017
年：2017
卷：71
期：3
页码：405-414
全文大小：2537 K
卷排序：71

文摘

Metastatic renal cell carcinoma (RCC) patients are commonly treated with vascular endothelial growth factor (VEGF) inhibitors or mammalian target of rapamycin inhibitors. Correlations between somatic mutations and first-line targeted therapy outcomes have not been reported on a randomized trial.ObjectiveTo evaluate the relationship between tumor mutations and treatment outcomes in RECORD-3, a randomized trial comparing first-line everolimus (mTOR inhibitor) followed by sunitinib (VEGF inhibitor) at progression with the opposite sequence in 471 metastatic RCC patients.Design, setting, and participantsTargeted sequencing of 341 cancer genes at ∼540× coverage was performed on available tumor samples from 258 patients; 220 with clear cell histology (ccRCC).Outcome measurements and statistical analysisAssociations between somatic mutations and median first-line progression free survival (PFS1L) and overall survival were determined in metastatic ccRCC using Cox proportional hazards models and log-rank tests.Results and limitationsPrevalent mutations (≥ 10%) were VHL (75%), PBRM1 (46%), SETD2 (30%), BAP1 (19%), KDM5C (15%), and PTEN (12%). With first-line everolimus, PBRM1 and BAP1 mutations were associated with longer (median [95% confidence interval {CI}] 12.8 [8.1, 18.4] vs 5.5 [3.1, 8.4] mo) and shorter (median [95% CI] 4.9 [2.9, 8.1] vs 10.5 [7.3, 12.9] mo) PFS1L, respectively. With first-line sunitinib, KDM5C mutations were associated with longer PFS1L (median [95% CI] of 20.6 [12.4, 27.3] vs 8.3 [7.8, 11.0] mo). Molecular subgroups of metastatic ccRCC based on PBRM1, BAP1, and KDM5C mutations could have predictive values for patients treated with VEGF or mTOR inhibitors. Most tumor DNA was obtained from primary nephrectomy samples (94%), which could impact correlation statistics.ConclusionsPBRM1, BAP1, and KDM5C mutations impact outcomes of targeted therapies in metastatic ccRCC patients.Patient summaryLarge-scale genomic kidney cancer studies reported novel mutations and heterogeneous features among individual tumors, which could contribute to varied clinical outcomes. We demonstrated correlations between somatic mutations and treatment outcomes in clear cell renal cell carcinoma, supporting the value of genomic classification in prospective studies.