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首页> 外文期刊>Pathology oncology research: POR >Autologous dendritic cell based adoptive immunotherapy of patients with colorectal cancer - A phase i-ii study
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Autologous dendritic cell based adoptive immunotherapy of patients with colorectal cancer - A phase i-ii study

机译:大肠癌患者基于自体树突状细胞的过继免疫疗法-I-ii期研究

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Dendritic cell-based active immunotherapies of cancer patients are aimed to provoke the proliferation and differentiation of tumor-specific CD4+ and CD8+ T-lymphocytes towards protective effector cells. Isolation and in vitro differentiation of circulating blood monocytes has been established a reasonable platform for adoptively transferred DC-based immunotherapies. In the present study the safety and tolerability of vaccination by autologous tumor cell lysates (oncolysate)- or carcinoembriogenic antigen (CEA)-loaded DCs in patients with colorectal cancer was investigated in a phase I-II trial. The study included 12 patients with histologically confirmed colorectal cancer (Dukes B2-C stages). Six of the patients received oncolysate-pulsed, whereas the other six received recombinant CEA-loaded autologous DCs. The potential of the tumor antigen-loaded DCs to provoke the patient's immune system was studied both in vivo and in vitro. The clinical outcome of the therapy evaluated after 7 years revealed that none of the six patients treated with oncolysate-loaded DCs showed relapse of colorectal cancer, whereas three out of the six patients treated with CEA-loaded DCs died because of tumor relapse. Immunization with both the oncolysate- and the CEA-loaded autologous DCs induced measurable immune responses, which could be detected in vivo by cutaneous reactions and in vitro by lymphocyte proliferation assay. Our results show that vaccination by autologous DCs loaded with autologous oncolysates containing various tumor antigens represents a well tolerated therapeutic modality in patients with colorectal cancer without any detectable adverse effects. Demonstration of the efficacy of such therapy needs further studies with increased number of patients.
机译:癌症患者基于树突细胞的主动免疫疗法旨在引起肿瘤特异性CD4 +和CD8 + T淋巴细胞向保护性效应细胞的增殖和分化。循环血单核细胞的分离和体外分化已经为过继转移的基于DC的免疫疗法建立了合理的平台。在本研究中,在I-II期试验中研究了自体肿瘤细胞裂解液(癌溶解液)或致癌致癌抗原(CEA)加载的DC接种大肠癌患者的安全性和耐受性。该研究纳入了12例经组织学证实为大肠癌(Dukes B2-C分期)的患者。其中有6名患者接受了溶菌素脉冲治疗,而其他6名患者则接受了装载CEA的重组自体DC。在体内和体外研究了负载有肿瘤抗原的DCs激发患者免疫系统的潜力。经过7年的评估,该疗法的临床结果表明,接受溶酶裂解物DC治疗的6例患者均未显示出结直肠癌复发,而接受CEA的DC治疗的6例患者中有3例因肿瘤复发而死亡。用溶瘤产物和CEA负载的自体DC免疫均诱导了可测量的免疫反应,可以通过皮肤反应在体内检测到,而通过淋巴细胞增殖测定在体外检测到。我们的结果表明,载有多种肿瘤抗原的自体溶酶产物的自体DC接种疫苗在结直肠癌患者中具有良好的耐受性,且无任何可检测到的不良反应。此类疗法的疗效证明需要更多患者的进一步研究。

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