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一种新型抗体-白细胞介素 15 融合蛋白选择性定位于肿瘤,与 TNF 为基础的免疫细胞因子协同作用,并抑制转移。

A Novel Antibody-IL15 Fusion Protein Selectively Localizes to Tumors, Synergizes with TNF-based Immunocytokine, and Inhibits Metastasis.

机构信息

CiBIO (Department of Cellular, Computational and Integrative Biology), University of Trento, Povo, Trento, Italy.

Philochem AG, Otelfingen, Switzerland.

出版信息

Mol Cancer Ther. 2021 May;20(5):859-871. doi: 10.1158/1535-7163.MCT-20-0853. Epub 2021 Feb 25.

DOI:10.1158/1535-7163.MCT-20-0853
PMID:33632875
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7611336/
Abstract

IL15 is an immunostimulatory cytokine that holds promises for cancer therapy, but its performance (alone or as partner for fusion proteins) has often been limited by suboptimal accumulation in the tumor and very rapid clearance from circulation. Most recently, the Sushi Domain (SD, the shortest region of IL15 receptor α, capable of binding to IL15) has been fused to IL15-based anticancer products to increase its biological activity. Here, we describe two novel antibody fusion proteins (termed F8-F8-IL15 and F8-F8-SD-IL15), specific to the alternatively spliced EDA domain of fibronectin (a marker of tumor neoangiogenisis, expressed in the majority of solid and hematologic tumors, but absent in normal healthy tissues) and featuring the F8 antibody in single-chain diabody format (with a short linker between VH and VL, thus allowing the domains to pair with the complementary ones of another chain). Unlike previously described fusions of the F8 antibody with human IL15, F8-F8-IL15 and F8-F8-SD-IL15 exhibited a preferential uptake in solid tumors, as evidenced by quantitative biodistribution analysis with radioiodinated protein preparations. Both products were potently active against mouse metastatic colon carcinomas and in sarcoma lesion in combination with targeted TNF. The results may be of clinical significance, as F8-F8-IL15 and F8-F8-SD-IL15 are fully human proteins, which recognize the cognate tumor-associated antigen with identical affinity in mouse and man.

摘要

白细胞介素 15(IL-15)是一种免疫刺激细胞因子,在癌症治疗方面具有广阔的应用前景,但由于其在肿瘤中的积累效果不理想,且在体内循环中清除速度非常快,因此其性能(单独使用或与融合蛋白联合使用)常常受到限制。最近,Sushi 结构域(SD,IL-15 受体α的最短区域,能够与 IL-15 结合)已被融合到基于白细胞介素 15 的抗癌产品中,以增加其生物活性。在这里,我们描述了两种新型抗体融合蛋白(分别称为 F8-F8-IL15 和 F8-F8-SD-IL15),它们特异性地针对纤连蛋白的交替剪接 EDA 结构域(肿瘤新生血管形成的标志物,在大多数实体瘤和血液系统肿瘤中表达,但在正常健康组织中不存在),并采用单链二价抗体形式的 F8 抗体(在 VH 和 VL 之间有一个短的连接子,从而允许这些结构域与另一条链的互补结构域配对)。与之前描述的 F8 抗体与人白细胞介素 15 的融合不同,F8-F8-IL15 和 F8-F8-SD-IL15 表现出在实体瘤中优先摄取的特性,这可以通过用放射性碘标记蛋白制剂进行定量生物分布分析来证明。这两种产物在与靶向 TNF 联合使用时,对小鼠转移性结肠腺癌和肉瘤病变都具有很强的活性。这些结果可能具有临床意义,因为 F8-F8-IL15 和 F8-F8-SD-IL15 都是完全人源蛋白,它们在小鼠和人类中以相同的亲和力识别同源的肿瘤相关抗原。

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