Battaglia Alessandra, Fossati Marco, Buzzonetti Alexia, Scambia Giovanni, Fattorossi Andrea
Ist. Clinica Ostetrica e Ginecologica, Univ. Cattolica S. Cuore, Rome, Italy.
Polo Scienze della Salute della Donna e del Bambino, Fondazione Policlinico Gemelli, Rome, Italy.
Immunol Lett. 2017 Nov;191:35-39. doi: 10.1016/j.imlet.2017.09.006. Epub 2017 Sep 14.
Despite encouraging phase I and II study results, vaccination of ovarian cancer patients with abagovomab - an anti-idiotypic mAb that mimics the ovarian cancer CA125 protein - failed to demonstrate efficacy in the phase III trial named MIMOSA (NCT00418574). We postulated that in this trial patients with a more robust immune system did respond to abagovomab but went undetected among a larger number of non-responders. We also postulated that assessment of the immune system status ahead of abagovomab administration might predict patients' propensity to respond to abagovomab.
The immune system status was assessed as percentage and absolute count of CD8 T cells producing IFN-γ after stimulation with Staphylococcal Enterotoxin B (SEB) in 80 patients on abagovomab and 31 patients on placebo from the MIMOSA trial ahead of treatment. Optimal cutoffs of the two variables were calculated by the web application "Cutoff Finder" as the points with most significant (log-rank test) splits based on relapse-free survival (RFS). The Kaplan-Meier curves and log-rank test served to estimate and compare RFS in patients with percentage and absolute count of IFN-γ producing CD8 T cells around the cutoffs.
Patients on abagovomab with IFN-γ producing CD8T cell percentage above the cutoff had a better RFS (p=0.042) than those with IFN-γ producing CD8T cell percentage below the cutoff. Patients on abagovomab with IFN-γ producing CD8T cell absolute count above the cutoff had a better RFS (p=0.019) than those with IFN-γ producing CD8T cell absolute counts below the cutoff. Consistently, the RFS of patients on abagovomab with IFN-γ producing CD8T cell percentage and absolute counts values below the respective cutoffs was identical to that of patients on placebo. Neither the percentage nor the absolute count of IFN-γ producing CD8T cells correlated with RFS in patients on placebo.
A robust immune system is essential to obtain a clinical response in OC patients undergoing abagovomab immunotherapy whereas a robust immune system does not confer per se a survival advantage. Further work will clarify whether the results shown here apply only in the present setting or extend to other types of cancer and/or immunotherapeutic agents.
尽管I期和II期研究结果令人鼓舞,但用阿巴戈单抗(一种模拟卵巢癌CA125蛋白的抗独特型单克隆抗体)对卵巢癌患者进行疫苗接种,在名为MIMOSA(NCT00418574)的III期试验中未能证明其疗效。我们推测,在该试验中,免疫系统更强健的患者确实对阿巴戈单抗有反应,但在大量无反应者中未被检测到。我们还推测,在给予阿巴戈单抗之前评估免疫系统状态可能预测患者对阿巴戈单抗的反应倾向。
在MIMOSA试验中,对80例接受阿巴戈单抗治疗的患者和31例接受安慰剂治疗的患者,在治疗前用葡萄球菌肠毒素B(SEB)刺激后,评估其产生γ干扰素的CD8 T细胞的百分比和绝对计数,以此来评估免疫系统状态。通过网络应用程序“Cutoff Finder”计算这两个变量的最佳临界值,即基于无复发生存期(RFS)具有最显著(对数秩检验)差异的点。采用Kaplan-Meier曲线和对数秩检验来估计和比较临界值附近产生γ干扰素的CD8 T细胞百分比和绝对计数的患者的RFS。
接受阿巴戈单抗治疗且产生γ干扰素的CD8 T细胞百分比高于临界值的患者,其RFS(p = 0.042)优于产生γ干扰素的CD8 T细胞百分比低于临界值的患者。接受阿巴戈单抗治疗且产生γ干扰素的CD8 T细胞绝对计数高于临界值的患者,其RFS(p = 0.019)优于产生γ干扰素的CD8 T细胞绝对计数低于临界值的患者。同样,接受阿巴戈单抗治疗且产生γ干扰素的CD8 T细胞百分比和绝对计数均低于各自临界值的患者的RFS与接受安慰剂治疗的患者相同。在接受安慰剂治疗的患者中,产生γ干扰素的CD8 T细胞的百分比和绝对计数均与RFS无关。
强健的免疫系统对于接受阿巴戈单抗免疫治疗的卵巢癌患者获得临床反应至关重要,而强健的免疫系统本身并不能带来生存优势。进一步的研究将阐明此处所示结果是仅适用于当前情况,还是可扩展到其他类型的癌症和/或免疫治疗药物。
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