Department of Molecular Oncology, Cancer Institute (WIA), Dr. Krishnamurthy Campus, Chennai 600036, India.
Department of Radiation Oncology, Cancer Institute (WIA), Dr. Krishnamurthy Campus, Chennai 600036, India.
J Gynecol Oncol. 2021 Jul;32(4):e59. doi: 10.3802/jgo.2021.32.e59. Epub 2021 Apr 6.
Dendritic cells (DCs) are administered as immunotherapeutic adjuvants after the completion of standard treatment in most settings. However, our Phase I trial indicated that one patient out of four, who received autologous tumor lysate-pulsed dendritic cell (TLDC) also received cisplatin chemotherapy and experienced complete regression of her lung lesion, continuing to be disease free till date. Hence, the objective of our current study is to evaluate the sustenance or augmentation of immune responses when autologous human papillomavirus positive cervical tumor lysate pulsed DC- are combined with cisplatin, using co-culture assays in vitro.
Before treatment, peripheral blood and punch biopsy samples were collected from 23 cervical cancer patients after obtaining an informed consent. DC functionality was confirmed through phenotypic and functional assays using autologous peripheral blood mononuclear cells as responders. For cisplatin experiments, the drug was added at 150, 200 (clinical dose equivalent), and 400 μM concentrations to DCs alone or DC-T cell co-cultures. Phenotypic assessment and functional characterization of DCs was done using flow cytometry. Cytokine enzyme-linked immunosorbent assay and interferon (IFN)-γ enzyme-linked immune absorbent spot assays were also performed.
The functionality of TLDCs was not compromised upon cisplatin treatment in vitro even at the highest (400 μM) concentration. Even though cisplatin treatment reduced the secretion of IFN-γ and interleukin (IL)-12p40 in co-cultures stimulated with TLDCs, this effect was not significant (p>0.05). A doubling of IFN-γ secretion following cisplatin treatment was observed in at least one of three independent experiments. Additional experiments showed a reduction in both FOXP3+ regulatory T cells and IL-10 levels.
Our results provide evidence that cisplatin treatment may be given after autologous TLDC administration to maintain or improve a productive anti-tumor response in vaccinated patients.
在大多数情况下,树突状细胞(DCs)在完成标准治疗后作为免疫治疗佐剂给药。然而,我们的 I 期试验表明,在接受自体肿瘤裂解物脉冲树突状细胞(TLDC)治疗的四名患者中,有一名患者还接受了顺铂化疗,并使肺部病变完全消退,直到现在仍无疾病进展。因此,我们当前研究的目的是通过体外共培养试验评估当自体人乳头瘤病毒阳性宫颈肿瘤裂解物脉冲树突状细胞与顺铂联合使用时,免疫反应的维持或增强。
在获得知情同意后,从 23 名宫颈癌患者的外周血和皮肤活检样本中采集样本。通过使用自体外周血单核细胞作为应答者的表型和功能测定来确认 DC 的功能。对于顺铂实验,将药物分别以 150、200(临床剂量等效)和 400μM 浓度添加到单独的 DC 或 DC-T 细胞共培养物中。使用流式细胞术进行 DC 的表型评估和功能特征分析。还进行了细胞因子酶联免疫吸附试验和干扰素(IFN)-γ酶联免疫吸附斑点试验。
即使在最高(400μM)浓度下,TLDC 经顺铂处理后其功能也不会受到影响。尽管顺铂处理降低了 TLDC 刺激的共培养物中 IFN-γ和白细胞介素(IL)-12p40 的分泌,但这种作用并不显著(p>0.05)。在至少三个独立实验中的一个实验中观察到 IFN-γ分泌增加一倍。其他实验表明,FOXP3+调节性 T 细胞和 IL-10 水平均降低。
我们的结果提供了证据表明,在给予自体 TLDC 后可以给予顺铂治疗,以维持或改善接种患者的抗肿瘤反应。
