TARGETING ENDOGENOUS ANTIBODIES TO OVARIAN CARCINOMA

针对卵巢癌的内源性抗体

• 批准号: 6465181
• 负责人: MOO J CHO
• 金额: $ 15.91万
• 依托单位: UNIV OF NORTH CAROLINA CHAPEL HILL
• 依托单位国家: 美国
• 财政年份: 2002
• 资助国家: 美国
• 起止时间: 2002-04-01 至 2004-03-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6465181
• 关键词: antitumor antibody; clone cells; folate; galactose; galactosyltransferases; gene targeting; genetically modified animals; humoral immunity; immunoconjugates; laboratory mouse; neoplasm /cancer immunology; neoplasm /cancer immunotherapy; nonhuman therapy evaluation; ovary neoplasms; receptor binding; vitamin receptor

DESCRIPTION (provided by applicant): Humans and Old World primates naturally produce a significant amount of antibodies which recognize a particular galactosyl epitope, GAL alpha 1-3GAL. We have been interested in testing if these anti-Gal antibodies can be targeted to undesirable cancerous cells. Specifically we wish to explore a possibility of redirecting these endogenous antibodies to ovarian carcinoma cells which overexpress folate receptor isotype alpha (FR-alpha) by means of chemical conjugates of folic acid to the galactosyl epitope. The end result should be the cytolysis of the target cell. Towards this goal, the present application is concerned with the total synthesis of the folate-digalactose conjugates and development of an ovarian cancer model in immune competent mice. Preparation of the conjugate which can mediate anti-Gal binding to FR+ cells with high avidity is the main chemistry goal of the project. Our strategy is to introduce multiple copies, 2 and 4 copies, of the epitopes to one molecule of folic acid at an optimal distance between them. Chemical synthesis will be carried out on a solid-phase support. The conjugates will be tested with FR+/Gal- human nasopharyngeal carcinoma KB cells for their ability of promoting the anti-Gal binding to FR on the cell surface. Specificity of the interaction will be tested in the presence of free folic acid or free disaccharide as well as with a conjugate that contains lactose instead of GAL alpha 1-3GAL. The antibody binding will be conveniently characterized by means of FACS procedure. The biological goal of this project is to develop a mouse model of ovarian cancer that is suitable for testing anti-tumor activity of our folate conjugates in vivo. Since normal mice express the galactosyl epitopes in their tissue, we will have to use alpha 1,3-GALactosyltransferase-knockout (GT/KO) mice. It is known that GT/KO mice produce anti-Gal as in humans. We plan to transform the ovarian epithelial cells harvested from these mice in culture to tumor-forming cell lines following a procedure we have recently developed. They will be then transfected with murine cDNA encoding full length FR-alpha. Finally these GAL-/FR+cells will be introduced into peritoneum of healthy GT/KO mice. Our current approach to immunotherapy of ovarian cancer is unique in that we are using naturally occurring endogenous antibodies. Immune modulators in this application are all small molecules with MW < 3 kDa, rendering pharmacokinetic properties most favorable for sustained activity in peritoneal cavity as well as reduced potential side effects.

描述（由申请人提供）： 人类和旧大陆灵长类动物自然产生大量 识别特定半乳糖基表位 GAL α 1-3GAL 的抗体。 我们一直有兴趣测试这些抗 Gal 抗体是否可以 针对不良癌细胞。具体来说，我们希望探索一个 将这些内源性抗体重新定向至卵巢癌的可能性 通过以下方式过表达叶酸受体同种型 α (FR-α) 的细胞 叶酸与半乳糖基表位的化学缀合物。最终结果 应该是靶细胞的细胞溶解。为实现这一目标，目前 应用涉及叶酸-双半乳糖的全合成 免疫活性卵巢癌模型的结合物和开发 老鼠。 介导抗Gal与FR+细胞结合的缀合物的制备 具有高亲和力是该项目的主要化学目标。 我们的策略是 将表位的多个拷贝（2 个和 4 个拷贝）引入一个分子 叶酸在它们之间的最佳距离。化学合成将 在固相支持物上进行。将用以下方法测试缀合物 FR+/Gal-人鼻咽癌KB细胞的促进能力 抗 Gal 抗体与细胞表面的 FR 结合。相互作用的特异性 还将在游离叶酸或游离二糖存在的情况下进行测试 与含有乳糖而不是 GAL α 1-3GAL 的缀合物一样。这 通过 FACS 可以方便地表征抗体结合 程序。 该项目的生物学目标是开发小鼠卵巢模型 适合测试叶酸抗肿瘤活性的癌症 体内缀合物。由于正常小鼠在其体内表达半乳糖基表位 组织，我们将不得不使用 α 1,3-GAL 乳糖基转移酶敲除 (GT/KO) 老鼠。众所周知，GT/KO 小鼠与人类一样产生抗 Gal 抗体。我们计划 将从这些小鼠培养物中收获的卵巢上皮细胞转化为 肿瘤形成细胞系遵循我们最近开发的程序。 然后用编码全长 FR-α 的鼠 cDNA 转染它们。 最后这些GAL-/FR+细胞将被引入健康的腹膜中 GT/KO 小鼠。 我们目前的卵巢癌免疫治疗方法是独特的，因为我们 正在使用天然存在的内源性抗体。免疫调节剂在这 应用均为MW < 3 kDa的小分子，呈现药代动力学 也最有利于腹膜腔持续活动的特性 减少潜在的副作用。