Efficacy and safety of anti-PD1 monotherapy or in combination with ipilimumab after BRAF/MEK inhibitors in patients with BRAF mutant metastatic melanoma

被引:10
|
作者
Pires da Silva, Ines [1 ,2 ,3 ]
Zakria, Danny [4 ]
Ahmed, Tasnia [1 ]
Trojanello, Claudia [5 ]
Dimitriou, Florentia [6 ]
Allayous, Clara [7 ]
Gerard, Camille [8 ]
Zimmer, Lisa [9 ]
Lo, Serigne [1 ]
Michielin, Olivier [8 ]
Lebbe, Celeste [10 ]
Mangana, Johanna [6 ]
Ascierto, Paolo Antonio [5 ]
Johnson, Douglas B. [4 ]
Carlino, Matteo [1 ,3 ]
Menzies, Alexander [1 ,2 ,11 ]
Long, Georgina [1 ,2 ,11 ]
机构
[1] Univ Sydney, Melanoma Inst Australia, Sydney, NSW, Australia
[2] Univ Sydney, Fac Med & Hlth, Sydney, NSW, Australia
[3] Blacktown & Westmead Hosp, Sydney, NSW, Australia
[4] Vanderbilt Univ, Med Ctr, Nashville, TN USA
[5] Ist Nazl Tumori IRCCS Fdn Pascale, Unit Melanoma Canc Immunotherapy & Dev Therapeut, Naples, Italy
[6] Univ Hosp Zurich, Dept Dermatol, Zurich, Switzerland
[7] Hop St Louis, AP HP, INSERM, Dermatolooncol,U976, Paris, France
[8] CHU Vaudois, Precis Oncol Ctr, Lausanne, Switzerland
[9] Univ Duisburg Essen, Univ Hosp Essen, Dept Dermatol, Essen, Germany
[10] Univ Paris Cite, Hop St Louis, AP HP, INSERM,U976,Dermatolooncol, Paris, France
[11] Royal North Shore & Mater Hosp, Sydney, NSW, Australia
基金
澳大利亚国家健康与医学研究理事会;
关键词
melanoma; immunotherapy; ADJUVANT PEMBROLIZUMAB; DOUBLE-BLIND; NIVOLUMAB; IMMUNOTHERAPY; DOCETAXEL; SURVIVAL; THERAPY;
D O I
10.1136/jitc-2022-004610
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background Patients with V600BRAF mutant metastatic melanoma have higher rates of progression-free survival (PFS) and overall survival (OS) with first-line anti-PD1 (PD1]+anti-CTLA-4 (IPI) versus PD1. Whether this is also true after BRAF/MEKi therapy is unknown. We aimed to determine the efficacy and safety of PD1 versus IPI +PD1 after BRAF/MEK inhibitors (BRAF/MEKi). Methods Patients with V600BRAF mutant metastatic melanoma treated with BRAF/MEKi who had subsequent PD1 versus IPI+PD1 at eight centers were included. The endpoints were objective response rate (ORR), PFS, OS and safety in each group. Results Of 200 patients with V600E (75%) or non-V600E (25%) mutant metastatic melanoma treated with BRAF/MEKi (median time of treatment 7.6 months; treatment cessation due to progressive disease in 77%), 115 (57.5%) had subsequent PD1 and 85 (42.5%) had IPI+PD1. Differences in patient characteristics between PD1 and IPI+PD1 groups included, age (med. 63 vs 54 years), time between BRAF/MEKi and PD1 +/- IPI (16 vs 4 days), Eastern Cooperative Oncology Group Performance Status (ECOG PS) of >= 1 (62% vs 44%), AJCC M1C/M1D stage (72% vs 94%) and progressing brain metastases at the start of PD1 +/- IPI (34% vs 57%). Median follow-up from PD1 +/- IPI start was 37.8 months (95% CI, 33.9 to 52.9). ORR was 36%; 34% with PD1 vs 39% with IPI+PD1 (p=0.5713). Median PFS was 3.4 months; 3.4 with PD1 vs 3.6 months with IPI+PD1 (p=0.6951). Median OS was 15.4 months; 14.4 for PD1 vs 20.5 months with IPI+PD1 (p=0.2603). The rate of grade 3 or 4 toxicities was higher with IPI+PD1 (31%) vs PD1 (7%). ORR, PFS and OS were numerically higher with IPI+PD1 vs PD1 across most subgroups except for females, those with <10 days between BRAF/MEKi and PD1 +/- IPI, and those with stage III/M1A/M1B melanoma. The combination of ECOG PS=0 and absence of liver metastases identified patients with >3 years OS (area under the curve, AUC=0.74), while ECOG PS >= 1, progressing brain metastases and presence of bone metastases predicted primary progression (AUC=0.67). Conclusions IPI+PD1 and PD1 after BRAF/MEKi have similar outcomes despite worse baseline prognostic features in the IPI+PD1 group, however, IPI+PD1 is more toxic. A combination of clinical factors can identify long-term survivors, but less accurately those with primary resistance to immunotherapy after targeted therapy.
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页数:9
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