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纳米抗体-铁蛋白偶联物用于靶向光动力疗法。

Nanobody-Ferritin Conjugate for Targeted Photodynamic Therapy.

机构信息

Department of Chemistry, CAS Key Laboratory of, Soft Mater Chemistry, University of Science and Technology of China, 96 Jinzhai Road, Hefei, Anhui, 230026, P. R. China.

出版信息

Chemistry. 2020 Jun 10;26(33):7442-7450. doi: 10.1002/chem.202000075. Epub 2020 May 19.

DOI:10.1002/chem.202000075
PMID:32166771
Abstract

Ferritin is an iron-storage protein nanocage that is assembled from 24 subunits. The hollow cavity of ferritin enables its encapsulation of various therapeutic agents; therefore, ferritin has been intensively investigated for drug delivery. The use of antibody-ferritin conjugates provides an effective approach for targeted drug delivery. However, the complicated preparation and limited protein stability hamper wide applications of this system. Herein, we designed a novel nanobody-ferritin platform (Nb-Ftn) for targeted drug delivery. The site-specific conjugation between nanobody and ferritin is achieved by transglutaminase-catalyzed protein ligation. This ligation strategy allows the Nb conjugation after drug loading in ferritin, which avoids deactivation of the nanobody under the harsh pH environment required for drug encapsulation. To verify the tumor targeting of this Nb-Ftn platform, a photodynamic reagent, manganese phthalocyanine (MnPc), was loaded into the ferritin cavity, and an anti-EGFR nanobody was conjugated to the surface of the ferritin. The ferritin nanocage can encapsulate about 82 MnPc molecules. This MnPc@Nb-Ftn conjugate can be efficiently internalized by EGFR positive A431 cancer cells, but not by EGFR negative MCF-7 cells. Upon 730 nm laser irradiation, MnPc@Nb-Ftn selectively killed EGFR positive A431 cells by generating reactive oxygen species (ROS), whereas no obvious damage was observed on MCF-7 cells. Given that ferritin can be used for encapsulation of various therapeutic agents, this work provides a strategy for facile construction of nanobody-ferritin for targeted drug delivery.

摘要

铁蛋白是一种由 24 个亚基组装而成的铁储存蛋白纳米笼。铁蛋白的空心腔使其能够封装各种治疗剂;因此,铁蛋白已被广泛研究用于药物递送。抗体-铁蛋白缀合物的使用为靶向药物递送提供了一种有效方法。然而,复杂的制备和有限的蛋白质稳定性阻碍了该系统的广泛应用。在这里,我们设计了一种用于靶向药物递送的新型纳米体-铁蛋白平台 (Nb-Ftn)。纳米体和铁蛋白之间的特异性连接是通过转谷氨酰胺酶催化的蛋白质连接实现的。这种连接策略允许在铁蛋白中加载药物后进行纳米体缀合,从而避免了在药物包封所需的苛刻 pH 环境下纳米体失活。为了验证该 Nb-Ftn 平台的肿瘤靶向性,将光动力试剂锰酞菁 (MnPc) 载入铁蛋白腔中,并将抗 EGFR 纳米体缀合到铁蛋白表面。铁蛋白纳米笼可以封装约 82 个 MnPc 分子。这种 MnPc@Nb-Ftn 缀合物可以被 EGFR 阳性 A431 癌细胞有效内化,但不能被 EGFR 阴性 MCF-7 细胞内化。在 730nm 激光照射下,MnPc@Nb-Ftn 通过产生活性氧 (ROS) 选择性杀死 EGFR 阳性 A431 细胞,而对 MCF-7 细胞没有明显损伤。鉴于铁蛋白可用于封装各种治疗剂,这项工作为构建用于靶向药物递送的纳米体-铁蛋白提供了一种简便的策略。

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