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化学免疫疗法可诱导自发性乳腺癌发生小鼠模型中的肿瘤消退。

Chemo-immunotherapy induces tumor regression in a mouse model of spontaneous mammary carcinogenesis.

作者信息

Aricò Eleonora, Sestili Paola, Carpinelli Giulia, Canese Rossella, Cecchetti Serena, Schiavoni Giovanna, D'Urso Maria Teresa, Belardelli Filippo, Proietti Enrico

机构信息

Department of Haematology, Oncology and Molecular Medicine, Istituto Superiore di Sanità, Rome, Italy.

Department of Cell Biology and Neurosciences, Istituto Superiore di Sanità, Rome, Italy.

出版信息

Oncotarget. 2016 Sep 13;7(37):59754-59765. doi: 10.18632/oncotarget.10880.

Abstract

Tumor-specific immune tolerance represents an obstacle for the development of effective anti-tumor immune responses through cancer vaccines. We here evaluated the efficacy of chemo-immunotherapy in breaking tumor-specific immune tolerance in an almost incurable mouse model of spontaneous carcinogenesis.Transgenic HER-2/neu mice bearing large mammary tumors received the adoptive transfer of splenocytes and serum isolated from immune donors, with or without pre-conditioning with cyclophosphamide. Treatment efficacy was assessed by monitoring tumor growth by manual inspection and by magnetic resonance imaging. The same chemo-immunotherapy protocol was tested on tumor-free HER-2/neu mice, to evaluate the effects on tumor emergence.Our data show that chemo-immunotherapy hampered carcinogenesis and caused the regression of large mammary tumor lesions in tumor-bearing HER-2/neu mice. The complete eradication of a significant number of tumor lesions occurred only in mice receiving cyclophosphamide shortly before immunotherapy, and was associated with increased serum anti HER-2/p185 antibodies and tumor leukocyte infiltration. The same protocol significantly delayed the appearance of mammary tumors when administered to tumor-free HER-2/neu mice, indicating that this chemo-immunotherapy approach acted through the elicitation of an effective anti-tumor immune response. Overall, our data support the immune-modulatory role of chemotherapy in overcoming cancer immune tolerance when administered at lymphodepleting non-myeloablative doses shortly before transfer of antigen-specific immune cells and immunoglobulins. These findings open new perspectives on combining immune-modulatory chemotherapy and immunotherapy to overcome immune tolerance in cancer patients.

摘要

肿瘤特异性免疫耐受是通过癌症疫苗产生有效的抗肿瘤免疫反应的障碍。我们在此评估了化学免疫疗法在一种几乎无法治愈的自发致癌小鼠模型中打破肿瘤特异性免疫耐受的疗效。携带大乳腺肿瘤的转基因HER-2/neu小鼠接受了从免疫供体分离的脾细胞和血清的过继转移,同时或不进行环磷酰胺预处理。通过手动检查和磁共振成像监测肿瘤生长来评估治疗效果。在无肿瘤的HER-2/neu小鼠上测试相同的化学免疫疗法方案,以评估对肿瘤发生的影响。我们的数据表明,化学免疫疗法阻碍了致癌作用,并导致携带肿瘤的HER-2/neu小鼠的大乳腺肿瘤病变消退。仅在免疫治疗前不久接受环磷酰胺的小鼠中,大量肿瘤病变被完全根除,这与血清抗HER-2/p185抗体增加和肿瘤白细胞浸润有关。当给予无肿瘤的HER-2/neu小鼠时,相同的方案显著延迟了乳腺肿瘤的出现,表明这种化学免疫疗法通过引发有效的抗肿瘤免疫反应起作用。总体而言,我们的数据支持化疗在抗原特异性免疫细胞和免疫球蛋白转移前不久以淋巴细胞清除但非骨髓消融剂量给药时,在克服癌症免疫耐受方面的免疫调节作用。这些发现为联合免疫调节化疗和免疫疗法以克服癌症患者的免疫耐受开辟了新的前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c08/5312346/ea0c13f5a83f/oncotarget-07-59754-g001.jpg

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