Meeting
2017 ASCO Annual Meeting
Relapse-free survial and target identification to enhance response with neoadjuvant and adjuvant dabrafenib + trametinib (D+T) treatment compared to standard-of-care (SOC) surgery in patients (pts) with high-risk resectable BRAF-mutant metastatic melanoma.
Authors
Jennifer Ann Wargo
The University of Texas MD Anderson Cancer Center, Houston, TX
Jennifer Ann Wargo , Rodabe Navroze Amaria , Peter A. Prieto , Miles Cameron Andrews , Michael T. Tetzlaff , Phillip Andrew Futreal , Patrick Hwu , Wen-Jen Hwu , Isabella Claudia Glitza , Hussein Abdul-Hassan Tawbi , Janice N. Cormier , Jeffrey Edwin Lee , Sapna Pradyuman Patel , Lauren Simpson , Elizabeth M. Burton , Roland L. Bassett Jr., Merrick I. Ross , Jeffrey E. Gershenwald , Michael A. Davies , Scott Eric Woodman
Organizations
The University of Texas MD Anderson Cancer Center, Houston, TX, Austin Hospital, Victoria, Australia, MD Anderson Cancer Center, Houston, TX, The University of Texas, Houston, TX
Research Funding
Pharmaceutical/Biotech Company
Background: Targeted and immune therapies have dramatically improved outcomes in stage IV metastatic melanoma pts. These agents are now being tested in earlier-stage disease. SOC surgery for high-risk resectable melanoma (AJCC stage IIIB/IIIC), with or without adjuvant therapy, is associated with a high risk of relapse (~70%). We hypothesized that neoadjuvant (neo) + adjuvant treatment with D+T improves RFS in these pts. Longitudinally collected biospecimens from pts receiving this treatment were analyzed to identify candidate strategies to further improve outcomes. Methods: A prospective single-institution randomized clinical trial (NCT02231775) was conducted in BRAF-mutant pts with resectable Stage IIIB/C or oligometastatic stage IV melanoma. Pts were randomized 1:2 to SOC (Arm A) versus neo + adjuvant D+T (Arm B; 8 wks neo + 44 wks adjuvant). The primary endpoint was RFS. Tumor biopsies were collected at baseline, week 3, and at surgery for molecular and immune profiling (whole exome sequencing, gene expression profiling, IHC, flow cytometry). Results: 21 of a planned 84 patients were enrolled (Arm A = 7, Arm B = 14). Arms were well balanced for standard prognostic factors, and toxicity was manageable. RECIST response rate with neo D+T was 77%, and the pathologic complete response rate (pCR) was 58%. First interim analysis revealed significantly improved RFS in the D+T arm over SOC (HR 62.5, p < 0.0001), leading to early closure to enrollment. Pts with a pCR at surgery had significantly improved RFS versus pts without pCR (p = 0.04) on neo D+T. Tumor profiling revealed incomplete MAPK pathway blockade and higher levels of CD8+ T cells expressing immunomodulators Tim-3 and Lag-3 in pts who did not achieve a pCR. Conclusions: Neo + adjuvant D+T is associated with a high pCR rate and markedly improved RFS over SOC in pts with high-risk resectable BRAF-mutant metastatic melanoma. pCR at surgery is associated with improved RFS. Tumor analyses reveal candidate targets for testing in future trials to enhance responses to neo D+T. Clinical trial information: NCT02231775
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Abstract Details
Session Type
Poster Session
Session Title
Melanoma/Skin Cancers
Track
Melanoma/Skin Cancers
Sub Track
Local-Regional Disease
Clinical Trial Registration Number
NCT02231775
Citation
J Clin Oncol 35, 2017 (suppl; abstr 9587)
DOI
10.1200/JCO.2017.35.15_suppl.9587
Abstract #
9587
Poster Bd #
195
Abstract Disclosures
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