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A randomized phase II study: CRS207/GVAX plus anti-PD1 and anti-CTLA4 recruits mesothelin- and mKRAS-specific T cells into PDAC

医学 易普利姆玛 无容量 克拉斯 免疫疗法 间皮素 免疫学 临床终点 免疫系统 癌症研究 黑色素瘤 髓样 免疫检查点 肿瘤微环境 肿瘤科 临床研究阶段 内科学 不利影响 进行性疾病 癌症 癌症免疫疗法 T细胞 化疗 FOXP3型
作者
Katherine M. Bever,Amanda Huff,Ludmila Danilova,Meredith Wetzel,Joseph A. Tandurella,Jennifer N. Durham,Tingchang Wang,Jae W. Lee,Erin Coyne,Janelle M. Montagne,Jacob T. Mitchell,Alexei Hernandez,Sarah M. Shin,Robert A. Anders,Hao Wang,Elana J. Fertig,Elizabeth M. Jaffee,Dung T. Le,W. Ho
出处
期刊:Cancer immunology research [American Association for Cancer Research]
标识
DOI:10.1158/2326-6066.cir-25-0545
摘要

Abstract Pancreatic ductal adenocarcinoma (PDAC) remains highly lethal and has poor immunogenicity, warranting the use of vaccines to guide and recruit the immune response. Building on prior efforts to achieve clinical immunotherapeutic responses against PDAC, we conducted a phase II study (NCT03190265) that combined attenuated mesothelin-secreting listeria vaccine (CRS-207) and GM-CSF–secreting allogeneic whole-cell vaccine (GVAX) along with checkpoint inhibition. Patients with metastatic PDAC who progressed on chemotherapy were enrolled in one of two treatment arms in a randomized fashion. CRS-207 was given with anti-PD1 (nivolumab) and anti-CTLA4 (ipilimumab) with (Arm A) or without (Arm B) GVAX. Primary endpoint was objective response rate (ORR) and the secondary endpoint was safety. 57 patients received at least one dose of treatment, with 2 partial responses (4% ORR), both Arm B. The response rates were not significantly different between the two arms. Related grade ≥3 adverse events were seen in 39 (68%) patients, including 33 events attributed to CRS-207. Mass cytometry analysis of serially obtained biospecimens demonstrated treatment-induced promotion of T-cell memory and infiltration into the tumor microenvironment (TME). Peptide-specific T-cell expansions in vitro followed by T-cell receptor sequencing revealed clones specific to mesothelin and mutant KRAS within the tumor. Accompanying these antitumor T-cell responses was significant enrichment of myeloid cells. High myeloid and Treg signatures correlated with poor responses. We conclude that GVAX/CRS-207 plus nivolumab and ipilimumab successfully generates and expands T-cell clones specific to mesothelin and mutant KRAS within the PDAC TME but immunotherapy-induced myeloid-cell enrichment remains a barrier to greater efficacy.

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