Glioblastoma-mediated Immune Dysfunction Limits CMV-specific T Cells and Therapeutic Responses: Results from a Phase I/II Trial

白细胞清除术 替莫唑胺 医学 CD8型 免疫学 免疫系统 细胞毒性T细胞 免疫疗法 抗原 内科学 化疗 胃肠病学 生物 川地34 体外 生物化学 遗传学 干细胞
作者
Shiao-Pei Weathers,Marta Penas‐Prado,Be-Lian Pei,Xiaoyang Ling,Cynthia Kassab,Pinaki P. Banerjee,Mustafa Bdiwi,Hila Shaim,Abdullah Alsuliman,Mayra Shanley,John de Groot,Barbara O’Brien,Rebecca A. Harrison,Nazanin Majd,Carlos Kamiya-Matsuoka,Gregory N. Fuller,Jason T. Huse,Linda Chi,Ganesh Rao,Jeffrey S. Weinberg
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:26 (14): 3565-3577 被引量:42
标识
DOI:10.1158/1078-0432.ccr-20-0176
摘要

Cytomegalovirus (CMV) antigens occur in glioblastoma but not in normal brains, making them desirable immunologic targets.Highly functional autologous polyclonal CMV pp65-specific T cells from patients with glioblastoma were numerically expanded under good manufacturing practice compliant conditions and administered after 3 weeks of lymphodepleting dose-dense temozolomide (100 mg/m2) treatment. The phase I component used a 3+3 design, ascending through four dose levels (5 × 106-1 × 108 cells). Treatment occurred every 6 weeks for four cycles. In vivo persistence and effector function of CMV-specific T cells was determined by dextramer staining and multiparameter flow cytometry in serially sampled peripheral blood and in the tumor microenvironment.We screened 65 patients; 41 were seropositive for CMV; 25 underwent leukapheresis; and 20 completed ≥1 cycle. No dose-limiting toxicities were observed. Radiographic response was complete in 1 patient, partial in 2. Median progression-free survival (PFS) time was 1.3 months [95% confidence interval (CI), 0-8.3 months]; 6-month PFS was 19% (95% CI, 7%-52%); and median overall survival time was 12 months (95% CI, 6 months to not reached). Repeated infusions of CMV-T cells paralleled significant increases in circulating CMV+ CD8+ T cells, but cytokine production showing effector activity was suppressed, especially from T cells obtained directly from glioblastomas.Adoptive infusion of CMV-specific T cells after lymphodepletion with dose-dense temozolomide was well tolerated. But apparently CMV seropositivity does not guarantee tumor susceptibility to CMV-specific T cells, suggesting heterogeneity in CMV antigen expression. Moreover, effector function of these T cells was attenuated, indicating a requirement for further T-cell modulation to prevent their dysfunction before conducting large-scale clinical studies.
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