Department of Oncology, Emek Medical Center, Afula.
Department of Epidemiology, Biostatistics, and Community Health Sciences, School of Public Health, Ben Gurion University of the Negev, Beer Sheba.
J Immunother. 2024 May 1;47(4):117-122. doi: 10.1097/CJI.0000000000000493. Epub 2023 Nov 1.
Metabolic pathways may regulate responses to cancer immunotherapy (IO). Due to its immunomodulatory properties, we sought to examine the association between serum vitamin B12 (VitB12) and survival in individuals with cancer treated with immune checkpoint inhibitors, compared with biological and chemotherapy. We collected data on patients with advanced cancer initiating intravenous antineoplastic treatment and a concomitant VitB12 measurement (elevated: >820 ng/L), between January 2010 and January 2022. Patients on IO and other regimens (control) were compared using the Mann-Whitney test for continuous variables, χ 2 test or Fisher test for categorical variables, and multivariate Cox regression models assessed the effect of VitB12 on overall survival and progression-free survival, adjusting for confounders. Patient groups (control: n = 408; IO: n = 93) were balanced for the treatment line and VitB12 (elevated 29.9% vs 23.7%; mean 762.4 vs 687.6 ng/L). In multivariate analysis, overall survival in all patients was negatively associated with VitB12 [control: hazard ratio (HR): 1.4, 95% CI: 1.01-1.96, P = 0.04, false discovery rate (FDR): 0.069; IO: HR: 2.74 as sum of linear baseline and interaction effects, log scale], age (HR: 1.03, 95% CI: 1.02-1.04, P < 0.01), male sex (HR: 0.66, 95% CI: 0.50-0.88, P < 0.01), and neutrophil-to-lymphocyte ratio (HR: 1.05, 95% CI: 0.48-0.99, P = 0.01). However, VitB12 was significantly negatively associated with progression-free survival only in the IO group ( P < 0.001, FDR < 0.001, calculated HR: 8.34; biological treatment P = 0.08; FDR: 0.111; neutrophil-to-lymphocyte ratio, P = 0.07; FDR: 0.09). Taken together, elevated VitB12 was a negative predictor for outcomes on IO, independently of other known prognostic factors. Further research is needed to elucidate the immune-metabolic interplay and its interaction with the gut microbiome, as well as interventional strategies to enhance IO responses.
代谢途径可能调节癌症免疫治疗 (IO) 的反应。由于其免疫调节特性,我们试图研究血清维生素 B12 (VitB12) 与接受免疫检查点抑制剂治疗的癌症患者生存之间的关联,与生物和化疗相比。我们收集了 2010 年 1 月至 2022 年 1 月期间接受静脉抗肿瘤治疗和同时进行 VitB12 测量的晚期癌症患者的数据(升高:>820ng/L)。使用 Mann-Whitney 检验比较 IO 和其他方案(对照组)的患者连续变量,使用 χ 2 检验或 Fisher 检验比较分类变量,使用多变量 Cox 回归模型调整混杂因素后评估 VitB12 对总生存和无进展生存的影响。患者组(对照组:n=408;IO 组:n=93)在治疗线和 VitB12(升高 29.9%比 23.7%;平均 762.4 比 687.6ng/L)方面平衡。多变量分析显示,所有患者的总生存率与 VitB12 呈负相关[对照组:危险比(HR):1.4,95%CI:1.01-1.96,P=0.04,假发现率(FDR):0.069;IO 组:HR:2.74 为线性基线和交互效应之和,对数刻度]、年龄(HR:1.03,95%CI:1.02-1.04,P<0.01)、男性(HR:0.66,95%CI:0.50-0.88,P<0.01)和中性粒细胞与淋巴细胞比值(HR:1.05,95%CI:0.48-0.99,P=0.01)。然而,只有在 IO 组中,VitB12 与无进展生存期显著负相关(P<0.001,FDR<0.001,计算 HR:8.34;生物治疗 P=0.08;FDR:0.111;中性粒细胞与淋巴细胞比值,P=0.07;FDR:0.09)。总之,升高的 VitB12 是 IO 结果的负面预测因子,独立于其他已知的预后因素。需要进一步研究阐明免疫代谢相互作用及其与肠道微生物组的相互作用,以及增强 IO 反应的干预策略。
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