Prognostic impact of baseline tumour immune infiltrate on disease-free survival in patients with completely resected, BRAF<sup>v600</sup> mutation-positive melanoma receiving adjuvant vemurafenib.

Ascierto, P A; Lewis, K D; Di Giacomo, A M; Demidov, L; Mandalà, M; Bondarenko, I; Herbert, C; Mackiewicz, A; Rutkowski, P; Guminski, A; Simmons, B; Ye, C; Hooper, G; Wongchenko, M J; Goodman, G R; Yan, Y; Schadendorf, D

Prognostic impact of baseline tumour immune infiltrate on disease-free survival in patients with completely resected, BRAF^v600 mutation-positive melanoma receiving adjuvant vemurafenib.

Ascierto, P A; Lewis, K D; Di Giacomo, A M; Demidov, L; Mandalà, M; Bondarenko, I; Herbert, C; Mackiewicz, A; Rutkowski, P; Guminski, A; Simmons, B; Ye, C; Hooper, G; Wongchenko, M J; Goodman, G R; Yan, Y; Schadendorf, D.

Affiliation

Ascierto PA; Melanoma Unit, Cancer Immunotherapy and Development Therapeutics, Istituto Nazionale Tumori IRCCS Fondazione G. Pascale, Naples, Italy. Electronic address: p.ascierto@istitutotumori.na.it.
Lewis KD; Department of Medicine, University of Colorado Comprehensive Cancer Center, Aurora, Colorado, USA.
Di Giacomo AM; Division of Medical Oncology and Immunotherapy, University Hospital of Siena, Siena, Italy.
Demidov L; Department of Biotherapy, N. N. Blokhin Russian Cancer Research Center, Ministry of Health, Moscow, Russia.
Mandalà M; Department of Oncology and Haematology, Papa Giovanni XXIII Cancer Center Hospital, Bergamo, Italy.
Bondarenko I; Dnipropetrovsk State Medical Academy, Dnipropetrovsk, Ukraine.
Herbert C; Bristol Haematology and Oncology Centre, University Hospitals Bristol NHS Foundation Trust, Bristol, UK.
Mackiewicz A; Department of Cancer Immunology, Poznan University of Medical Sciences, Med-POLONIA, Poznan, Poland.
Rutkowski P; Department of Soft Tissue/Bone Sarcoma and Melanoma, Maria Sklodowska-Curie Institute - Oncology Center, Warsaw, Poland.
Guminski A; Melanoma Translational Research Group, Melanoma Institute Australia, Wollstonecraft, New South Wales, Australia.
Simmons B; Product Development Oncology, Genentech, Inc., South San Francisco, California, USA.
Ye C; Oncology Biostatistics, Genentech, Inc., South San Francisco, California, USA.
Hooper G; Clinical Development Department, Roche Products Ltd., Welwyn Garden City, UK.
Wongchenko MJ; Oncology Biomarker Development, Genentech, Inc., South San Francisco, California, USA.
Goodman GR; Safety Science Oncology, Genentech, Inc., South San Francisco, California, USA.
Yan Y; Oncology Biomarker Development, Genentech, Inc., South San Francisco, California, USA.
Schadendorf D; Department of Dermatology, Essen University Hospital, Essen, Germany; German Cancer Consortium, Heidelberg, Germany.

Ann Oncol ; 31(1): 153-159, 2020 01.

Article in En | MEDLINE | ID: mdl-31912791

ABSTRACT

BACKGROUND: We conducted a retrospective exploratory analysis to evaluate the effects of baseline tumour immune infiltrate on disease-free survival (DFS) outcomes in patients with fully resected stage IIC-IIIC melanoma receiving adjuvant vemurafenib monotherapy or placebo in the BRIM8 study. PATIENTS AND METHODS: BRIM8 was a phase III, international, double-blind, randomised, placebo-controlled study. Eligible patients with BRAFV600 mutation-positive, completely resected melanoma were randomly assigned to oral vemurafenib (960 mg twice daily) or matching placebo for 52 weeks. The primary end point was DFS. The association of CD8+ T-cell infiltration and programmed death ligand 1 (PD-L1) expression with DFS, as measured by immunohistochemistry, was explored retrospectively. RESULTS: Four hundred ninety-eight patients were randomly assigned to receive adjuvant vemurafenib (n = 250) or placebo (n = 248); tumour samples were available for biomarker analysis for approximately 60% of patients. In the pooled biomarker population, placebo-treated patients with <1% CD8+ T cells in the tumour centre had shorter median DFS than those with ≥1% CD8+ T cells (7.7 versus 47.8 months). DFS benefit from vemurafenib versus placebo was greater in patients with <1% CD8+ T cells [hazard ratio (HR) 0.56; 95% confidence interval (CI) 0.34-0.92) than in patients with ≥1% CD8+ T cells (HR 0.77; 95% CI 0.48-1.22). Likewise, median DFS was shorter among placebo-treated patients with <5% versus ≥5% PD-L1+ immune cells (IC) in the tumour (7.2 versus 47.8 months). A greater DFS benefit with vemurafenib versus placebo was observed in patients with <5% PD-L1+IC (HR 0.36; 95% CI 0.24-0.56) than in patients with ≥5% PD-L1+IC (HR 0.99; 95% CI 0.58-1.69). CONCLUSIONS: The presence of CD8+ T cells and PD-L1+IC are favourable prognostic factors for DFS. Treatment with adjuvant vemurafenib may overcome the poor DFS prognosis associated with low CD8+ T-cell count or PD-L1 expression. CLINICALTRIALS. GOV IDENTIFIER: NCT01667419.

Subject(s)

Melanoma; Proto-Oncogene Proteins B-raf; Disease-Free Survival; Humans; Melanoma/drug therapy; Melanoma/genetics; Mutation; Prognosis; Proto-Oncogene Proteins B-raf/genetics; Retrospective Studies; Vemurafenib/therapeutic use

Key words

adjuvant therapy; melanoma; vemurafenib

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Proto-Oncogene Proteins B-raf / Melanoma Type of study: Observational_studies / Prognostic_studies / Risk_factors_studies Limits: Humans Language: En Journal: Ann Oncol Journal subject: NEOPLASIAS Year: 2020 Type: Article

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