An engineered ultrahigh affinity bi-paratopic uPAR targeting agent confers enhanced tumor targeting

IF 3.5 2区生物学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY

Biotechnology and Bioengineering Pub Date : 2024-07-04 DOI:10.1002/bit.28790

Gerald M. Cherf, Robert B. Lee, Nishant Mehta, Claire Clifford, Kathleen Torres, James R. Kintzing, Jennifer R. Cochran

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Abstract

Urokinase-type plasminogen activator receptor (uPAR) is overexpressed on tumor cells in multiple types of cancer and contributes to disease progression and metastasis. In this work, we engineered a novel bi-paratopic uPAR targeting agent by fusing the binding domains of two native uPAR ligands: uPA and vitronectin, with a flexible peptide linker. The linker length was optimized to facilitate simultaneous engagement of both domains to their adjacent epitopes on uPAR, resulting in a high affinity and avid binding interaction. Furthermore, the individual domains were affinity-matured using yeast surface display and directed evolution, resulting in a bi-paratopic protein with affinity in the picomolar to femtomolar range. This engineered uPAR targeting agent demonstrated significantly enhanced tumor localization in mouse tumor models compared to the native uPAR ligand and warrants further investigation as a diagnostic and therapeutic agent for cancer.

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一种超高亲和力双伞uPAR靶向制剂可增强肿瘤靶向性。

尿激酶型纤溶酶原激活物受体（uPAR）在多种类型癌症的肿瘤细胞上过度表达，并导致疾病进展和转移。在这项工作中，我们通过将两种原生uPAR配体（uPA和玻璃连蛋白）的结合结构域与一个灵活的多肽连接体融合，设计出了一种新型的双paratopic uPAR靶向制剂。连接体的长度经过了优化，以促进两个结构域同时与uPAR上的相邻表位结合，从而产生高亲和力和狂热的结合相互作用。此外，还利用酵母表面展示和定向进化技术对单个结构域进行了亲和力成熟，从而得到了亲和力在皮摩尔到飞摩尔范围内的双准分子蛋白。与原生uPAR配体相比，这种工程化的uPAR靶向制剂在小鼠肿瘤模型中的肿瘤定位能力明显增强，值得作为癌症诊断和治疗药物进行进一步研究。

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

Biotechnology and Bioengineering 工程技术-生物工程与应用微生物

CiteScore

7.90

自引率

5.30%

发文量

280

审稿时长

2.1 months

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