在C3H小鼠中,采用基于新型白细胞介素12的免疫治疗方案治愈已形成的非免疫原性肿瘤SCC VII。
Cure of an established nonimmunogenic tumor, SCC VII, with a novel interleukin 12-based immunotherapy regimen in C3H mice.
作者信息
Mandpe Aditi H, Tsung Kangla, Norton Jeffrey A
机构信息
Department of Otolaryngology-Head and Neck Surgery, University of California, San Francisco, and the Surgical Service Veterans Affairs Medical Center, San Francisco, 94143-0342, USA.
出版信息
Arch Otolaryngol Head Neck Surg. 2003 Jul;129(7):786-92. doi: 10.1001/archotol.129.7.786.
OBJECTIVE
To develop a murine model of effective treatment with immunotherapy for established head and neck squamous cell carcinoma.
DESIGN
Prospective animal study. Subjects Female C3H mice, 8 to 12 weeks old.
INTERVENTIONS
A subcutaneous inoculation of 2 x 10(5) SCC VII cells in C3H mice was established for 7 to 12 days. Tests for concomitant immunity were performed, with and without interleukin 12 modification. Tumors were also tested for responsiveness to interleukin 12 (5 mice) and to cyclophosphamide followed by interleukin 12 (5 mice). SCC VII tumors in 24 mice were treated with interleukin 12 followed by cyclophosphamide and interleukin 12. Five mice with tumors treated with isotonic sodium chloride solution served as controls. Tumors were measured 3 to 4 times weekly, and cure was defined as complete regression of the tumor for at least 60 days. Cured mice were rechallenged with 2 x 10(5) SCC VII cells to verify antitumor immunity. Immunohistochemistry of regressing tumors was performed for CD4+ and CD8+ T cells.
RESULTS
Tumor-bearing mice easily developed second tumors when challenged with 2 x 10(5) tumor cells in the opposite flank. However, interleukin 12 treatment provided immunity to second tumors in 8 (100%) of 8 mice when started at day 4 and in 2 (40%) of 5 when treated from day 7. SCC VII did not respond to standard interleukin 12 or cyclophosphamide plus interleukin 12 therapy. Seventy-five percent of animals (18/24) treated with interleukin 12 followed by cyclophosphamide plus interleukin 12 were successfully cured, and all cured mice resisted subsequent challenge with SCC VII. Immunohistochemistry of regressed tumors showed an intense CD4+ and CD8+ infiltrate that was absent in the untreated and nonresponding tumors.
CONCLUSIONS
Nonimmunogenic SCC VII is a nonimmunogenic tumor that can be converted into an immunogenic tumor with interleukin 12 treatment. Additional treatment with cyclophosphamide plus interleukin 12 leads to complete regression in 75% of mice.
目的
建立一种用于已确诊的头颈部鳞状细胞癌免疫治疗有效治疗的小鼠模型。
设计
前瞻性动物研究。对象为8至12周龄的雌性C3H小鼠。
干预措施
在C3H小鼠皮下接种2×10⁵个SCC VII细胞,持续7至12天。进行了有无白细胞介素12修饰的伴随免疫测试。还测试了肿瘤对白细胞介素12(5只小鼠)以及环磷酰胺后接白细胞介素12(5只小鼠)的反应性。24只小鼠的SCC VII肿瘤先用白细胞介素12治疗,然后用环磷酰胺和白细胞介素12治疗。5只接受等渗氯化钠溶液治疗的肿瘤小鼠作为对照。每周测量肿瘤3至4次,治愈定义为肿瘤完全消退至少60天。对治愈的小鼠用2×10⁵个SCC VII细胞再次攻击以验证抗肿瘤免疫力。对消退肿瘤进行CD4⁺和CD8⁺T细胞的免疫组织化学检测。
结果
荷瘤小鼠在对侧腹用2×10⁵个肿瘤细胞攻击时很容易长出第二个肿瘤。然而,白细胞介素12治疗在第4天开始时能使8只小鼠中的8只(100%)对第二个肿瘤产生免疫,在第7天开始治疗时能使5只小鼠中的2只(40%)产生免疫。SCC VII对标准的白细胞介素12或环磷酰胺加白细胞介素12治疗无反应。先用白细胞介素12然后用环磷酰胺加白细胞介素12治疗的动物中有75%(18/24)成功治愈,所有治愈的小鼠都能抵抗随后SCC VII的攻击。消退肿瘤的免疫组织化学显示有强烈的CD4⁺和CD8⁺浸润,而未治疗和无反应的肿瘤中没有这种浸润。
结论
非免疫原性的SCC VII是一种非免疫原性肿瘤,用白细胞介素12治疗可将其转化为免疫原性肿瘤。环磷酰胺加白细胞介素12的额外治疗可使75%的小鼠肿瘤完全消退。
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