研究动态
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分子成像支持多特异性癌症抗体的开发。

Molecular imaging supports the development of multispecific cancer antibodies.

发表日期:2024 Sep 26
作者: Claudia A J van Winkel, Frank R Pierik, Adrienne H Brouwers, Derk Jan A de Groot, Elisabeth G E de Vries, Marjolijn N Lub-de Hooge
来源: Nature Reviews Clinical Oncology

摘要:

多特异性抗体是工程化抗体衍生物,可以结合两个或多个不同的表位或抗原。与单特异性抗体的混合物不同,多特异性抗体的结合特性使两个特定分子能够物理连接,这一特性在癌症治疗中具有重要应用。多特异性抗体领域充满活力并迅速扩展;迄今为止,已有15种多特异性抗体获批临床使用,其中11种获批用于肿瘤适应症,还有超过100种新抗体正在临床开发中。然而,巨大的挑战限制了多特异性抗体在癌症治疗中的应用,特别是实体瘤靶向效率低下和严重的副作用。 PET 和单光子发射 CT 成像都可以揭示放射性标记多特异性抗体的生物分布和复杂的药理学。本综述总结了从多特异性抗体的临床前和临床分子成像研究中获得的见解,重点关注其结构特性,例如分子量、形状、靶标特异性、亲和力和亲和力。还强调了与使用分子成像研究支持多特异性抗体疗法的临床开发相关的机会。© 2024。Springer Nature Limited。
Multispecific antibodies are engineered antibody derivatives that can bind to two or more distinct epitopes or antigens. Unlike mixtures of monospecific antibodies, the binding properties of multispecific antibodies enable two specific molecules to be physically linked, a characteristic with important applications in cancer therapy. The field of multispecific antibodies is highly dynamic and expanding rapidly; to date, 15 multispecific antibodies have been approved for clinical use, of which 11 were approved for oncological indications, and more than 100 new antibodies are currently in clinical development. Nevertheless, substantial challenges limit the applications of multispecific antibodies in cancer therapy, particularly inefficient targeting of solid tumours and substantial adverse effects. Both PET and single photon emission CT imaging can reveal the biodistribution and complex pharmacology of radiolabelled multispecific antibodies. This Review summarizes the insights obtained from preclinical and clinical molecular imaging studies of multispecific antibodies, focusing on their structural properties, such as molecular weight, shape, target specificity, affinity and avidity. The opportunities associated with use of molecular imaging studies to support the clinical development of multispecific antibody therapies are also highlighted.© 2024. Springer Nature Limited.