Role of antibody engineering in generation of derivatives starting from MOv19 MAb: 40 years of biological/therapeutic tools against folate receptor alfa.

Q2 Medicine

Antibody Therapeutics Pub Date : 2022-10-27 eCollection Date: 2022-10-01 DOI:10.1093/abt/tbac026

Barbara Frigerio, Matilde Montermini, Canevari Silvana, Mariangela Figini

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Abstract

In the 1980s, we developed and characterized numerous murine monoclonal antibodies (MAbs) directed against human tumor-associated antigens. This mini review is focused on the generation of derivatives of an anti-folate receptor α (FRα) MAbs, named MOv19, exploiting the antibody-engineering progresses in the last 40 years. The FRα location on the luminal surface of proliferating epithelial cells, inaccessible to circulation, versus its over-expression in the entire surface of numerous carcinomas suggested a role for anti-FRα MAbs in the diagnosis and/or treatment of solid tumors. Presently, two MOv19 derivatives are in clinical trials: a chimeric resurfaced version in an antibody-drug conjugate format (SORAYA trial, 2022) and the murine scFv in a second generation chimeric antigen receptor, CAR-T (Phase Ia, 2021). MOv19 and its derivatives could be considered a relevant example that well-characterized anti-tumor murine Mabs and antibody engineering could be combined to generate useful therapeutic tools.

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抗体工程在生成从 MOv19 MAb 开始的衍生物中的作用：针对叶酸受体 alfa 的生物/治疗工具 40 年。

20 世纪 80 年代，我们开发并鉴定了许多针对人类肿瘤相关抗原的鼠类单克隆抗体（MAbs）。这篇微型综述的重点是利用过去 40 年中抗体工程的进步，研制出抗叶酸受体α（FRα）MAbs 的衍生物，并命名为 MOv19。FRα位于增殖上皮细胞的管腔表面，无法进入血液循环，而它在许多癌细胞的整个表面过度表达，这表明抗 FRα MAbs 可在实体瘤的诊断和/或治疗中发挥作用。目前，有两种 MOv19 衍生物正在进行临床试验：一种是抗体-药物共轭物形式的嵌合再表面化版本（SORAYA 试验，2022 年），另一种是第二代嵌合抗原受体 CAR-T 中的鼠 scFv（Ia 期，2021 年）。MOv19 及其衍生物可被视为一个相关范例，说明特征明确的抗肿瘤小鼠 Mabs 与抗体工程相结合，可以产生有用的治疗工具。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Antibody Therapeutics Medicine-Immunology and Allergy

CiteScore

8.70

自引率

0.00%

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审稿时长

8 weeks