Prognostic impact of baseline tumour immune infiltrate on disease-free survival in patients with completely resected, BRAFv600 mutation-positive melanoma receiving adjuvant vemurafenib

被引:32
作者
Ascierto, P. A. [1 ]
Lewis, K. D. [2 ]
Di Giacomo, A. M. [3 ]
Demidov, L. [4 ]
Mandala, M. [5 ]
Bondarenko, I [6 ]
Herbert, C. [7 ]
Mackiewicz, A. [8 ]
Rutkowski, P. [9 ]
Guminski, A. [10 ]
Simmons, B. [11 ]
Ye, C. [12 ]
Hooper, G. [13 ]
Wongchenko, M. J. [14 ]
Goodman, G. R. [15 ]
Yan, Y. [14 ]
Schadendorf, D. [16 ,17 ]
机构
[1] Ist Nazl Tumori IRCCS Fdn G Pascale, Melanoma Unit, Canc Immunotherapy & Dev Therapeut, Naples, Italy
[2] Univ Colorado, Dept Med, Comprehens Canc Ctr, Aurora, CO USA
[3] Univ Hosp Siena, Div Med Oncol & Immunotherapy, Siena, Italy
[4] Minist Hlth, Dept Biotherapy, NN Blokhin Russian Canc Res Ctr, Moscow, Russia
[5] Papa Giovanni XXIII Canc Ctr Hosp, Dept Oncol & Haematol, Bergamo, Italy
[6] Dnipropetrovsk State Med Acad, Dnepropetrovsk, Ukraine
[7] Univ Hosp Bristol NHS Fdn Trust, Bristol Haematol & Oncol Ctr, Bristol, Avon, England
[8] Poznan Univ Med Sci, Dept Canc Immunol, Med POLONIA, Poznan, Poland
[9] Maria Sklodowska Curie Inst Oncol Ctr, Dept Soft Tissue Bone Sarcoma & Melanoma, Warsaw, Poland
[10] Melanoma Inst Australia, Melanoma Translat Res Grp, Wollstonecraft, NSW, Australia
[11] Genentech Inc, Prod Dev Oncol, San Francisco, CA 94080 USA
[12] Genentech Inc, Oncol Biostat, San Francisco, CA 94080 USA
[13] Roche Prod Ltd, Clin Dev Dept, Welwyn Garden City, Herts, England
[14] Genentech Inc, Oncol Biomarker Dev, San Francisco, CA 94080 USA
[15] Genentech Inc, Safety Sci Oncol, San Francisco, CA 94080 USA
[16] Essen Univ Hosp, Dept Dermatol, Essen, Germany
[17] German Canc Consortium, Heidelberg, Germany
来源
ANNALS OF ONCOLOGY | 2020年 / 31卷 / 01期
关键词
adjuvant therapy; melanoma; vemurafenib; STAGE-III; DIFFERENTIAL EXPRESSION; T-CELL; PD-L1; INHIBITORS; IPILIMUMAB;
D O I
10.1016/j.annonc.2019.10.002
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
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 BRAF(V600) 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.
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收藏
页码:153 / 159
页数:7
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