MECHANISMS OF ADENOVIRUS VACCINES FOR COLON CANCER

腺病毒疫苗治疗结肠癌的机制

• 批准号: 6300546
• 负责人: STEPHEN L. ECK
• 金额: $ 15.41万
• 依托单位: WISTAR INSTITUTE
• 依托单位国家: 美国
• 财政年份: 2000
• 资助国家: 美国
• 起止时间: 2000-01-01 至 2000-12-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6300546
• 关键词: Adenoviridae; active immunization; cell type; colon neoplasms; dosage; interleukin 2; laboratory mouse; neoplasm /cancer therapy; neoplasm /cancer vaccine; tumor antigens; vaccine development

The major goal of this project is to identify an optimal adenovirus- based vaccination strategy against homologue (mEGP) of the human colorectal carcinoma-associated GA733 antigen. Since mice express mEGP on normal tissues (similar to GA733 Ag in humans), this animal model allows testing of the vaccine in an immunologically tolerant host and evaluation of potential toxicity. These studies will optimize the ability of this vaccine to overcome tolerance to this tumor antigen in settings that closely mimic patients with colon cancer. Therefore, they will have an impact on the initial human clinical trial (see Project 3, Aim 2) and will provide the basis for the testing of improved human colon cancer vaccines in the near future. We have prepared an adenovirus-based mEGP vaccine and have already shown that it can induce tumor protection in the mouse when used in combination with interleukin-2 (IL-2). This is the basis for our proposed series of experiments. Our initial experiments will address issues of immediate clinical relevance, i.e., administration of the vaccine by a cutaneous route, the need for one versus two doses of the vaccine, and the appropriate use of cytokine. Having identified parameters that limit or enhance our vaccine in a subcutaneous tumor model, we will than address whether our vaccination strategy is effective against more advanced and metastatic disease. This will provide us with the opportunity to improve our vaccine by studying the effects of different booster strategies, the use of other cytokines and the use of functionally active fragments (from Project 1) of mEGP. Having optimized our vaccine, we will study its mechanism of action by defining the target cells through which the adenovirus elicits anti-mEGP immunity, the role of the adenoviral proteins in the induction of the immune response, and the cell types that contribute to the effectiveness of the immune response.

该项目的主要目标是确定最佳的腺病毒- 基于人类同源物（mEGP）的疫苗接种策略 结直肠癌相关 GA733 抗原。由于小鼠表达 mEGP 正常组织（类似于人类的 GA733 Ag），该动物模型允许 在免疫耐受宿主中测试疫苗并进行评估 的潜在毒性。这些研究将优化这一能力 疫苗可克服对这种肿瘤抗原的耐受性 与结肠癌患者非常相似。因此，他们将有一个 对初始人体临床试验的影响（参见项目 3，目标 2）并将 为改进的人类结肠癌疫苗的测试提供基础 在不久的将来。我们已经制备了基于腺病毒的 mEGP 疫苗 已经表明它可以在小鼠体内诱导肿瘤保护 与白细胞介素-2 (IL-2) 联合使用。这是我们的基础 提出的一系列实验。我们最初的实验将解决 与临床直接相关的问题，即药物的管理 通过皮肤途径接种疫苗，需要一剂或两剂 疫苗，以及适当使用细胞因子。确定参数后 在皮下肿瘤模型中限制或增强我们的疫苗，我们将 而不是解决我们的疫苗接种策略是否对更多的疾病有效 晚期和转移性疾病。这将为我们提供机会 通过研究不同加强剂的效果来改进我们的疫苗 策略、其他细胞因子的使用以及功能活性的使用 mEGP 的片段（来自项目 1）。优化我们的疫苗后，我们将 通过定义靶细胞来研究其作用机制 腺病毒引发抗 mEGP 免疫，腺病毒的作用 诱导免疫反应的蛋白质，以及诱导免疫反应的细胞类型 有助于免疫反应的有效性。