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在小鼠肝转移模型中,用牛痘结肠溶瘤物进行主动特异性免疫治疗可增强白细胞介素-2和α干扰素的免疫调节及抗肿瘤作用。

Active specific immunotherapy with vaccinia colon oncolysate enhances the immunomodulatory and antitumor effects of interleukin-2 and interferon alpha in a murine hepatic metastasis model.

作者信息

Arroyo P J, Bash J A, Wallack M K

机构信息

Department of Surgery, Mount Sinai Medical Center, Miami Beach, Florida 33140.

出版信息

Cancer Immunol Immunother. 1990;31(5):305-11. doi: 10.1007/BF01740939.

Abstract

The role of cytokines as primary or adjuvant antineoplastic agents has been well established. Interleukin-2 (IL-2) and the interferons have, particularly, proven to be effective antitumor agents when given alone, and seem to act synergistically on the eradication of metastases from immunogenic tumors. Active specific immunotherapy, in the form of viral oncolysates, has also shown effectiveness in cancer therapy. Bearing this in mind, we decided to combine these agents in an adjuvant triple regimen and compare their effectiveness to other treatments in terms of tumor burden and survival in a murine colon cancer hepatic metastases model. BALB/c mice were injected with CC-36, a weakly immunogenic murine colon adenocarcinoma, intrasplenically, to produce artificial liver metastases. The animals were divided into one control group and seven treatment groups receiving either vaccinia colon oncolysate (VCO), IL-2, interferon-alpha (IFN alpha) alone, or combinations of these agents. Half the animals were followed for survival and the other half were sacrificed at the end of the experiment for quantification of tumor burden. The blood of the sacrificed animals was utilized in a series of immunological tests in order to demonstrate the cytolytic potential of the peripheral blood lymphocytes (PBL) in each treatment group, as well as to characterize phenotypically the cells acting as effectors. The triple-adjuvant regimen group was by far the most effective treatment group, demonstrating 100% survival and a significant reduction in tumor burden when compared to other groups. Furthermore, the PBL from the animals in this group showed 69.4% lysis of the CC-36 target cells in vitro. These effector lymphocytes were characterized as ASMG1-/Lyt2.2+ cytolytic lymphocytes. We conclude that these lymphocytes were stimulated by the administration of VCO and further augmented by the immunomodulation of the cytokines given in the triple regimen, and that such a regimen might prove beneficial in the treatment of established hepatic metastases from weakly immunogenic tumors.

摘要

细胞因子作为主要或辅助抗肿瘤药物的作用已得到充分证实。特别是白细胞介素-2(IL-2)和干扰素,单独使用时已被证明是有效的抗肿瘤药物,并且在根除免疫原性肿瘤的转移灶方面似乎具有协同作用。以病毒溶瘤产物形式存在的主动特异性免疫疗法在癌症治疗中也显示出有效性。考虑到这一点,我们决定将这些药物联合用于辅助三联疗法,并在小鼠结肠癌肝转移模型中,就肿瘤负荷和生存率而言,将其有效性与其他治疗方法进行比较。将BALB/c小鼠经脾内注射CC-36(一种弱免疫原性的小鼠结肠腺癌)以产生人工肝转移。动物被分为一个对照组和七个治疗组,分别接受痘苗结肠溶瘤产物(VCO)、IL-2、α干扰素(IFNα)单独治疗或这些药物的组合治疗。一半动物观察生存率,另一半在实验结束时处死以定量肿瘤负荷。处死动物的血液用于一系列免疫学检测,以证明每个治疗组外周血淋巴细胞(PBL)的细胞溶解潜力,并从表型上对作为效应细胞的细胞进行特征分析。三联辅助疗法组是迄今为止最有效的治疗组,与其他组相比,显示出100%的生存率和肿瘤负荷的显著降低。此外,该组动物的PBL在体外对CC-36靶细胞的裂解率为69.4%。这些效应淋巴细胞被鉴定为ASMG1-/Lyt2.2+细胞溶解淋巴细胞。我们得出结论,这些淋巴细胞受到VCO给药的刺激,并通过三联疗法中给予的细胞因子的免疫调节作用进一步增强,并且这样的疗法可能被证明对治疗弱免疫原性肿瘤已形成的肝转移有益。

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