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研发一种抗体结合蛋白笼作为分子识别药物的模块化纳米平台。

Developing an antibody-binding protein cage as a molecular recognition drug modular nanoplatform.

机构信息

BioNanotechnology Research Center, Korea Research Institute of Bioscience and Biotechnology (KRIBB) Daejeon 305-806, Republic of Korea.

出版信息

Biomaterials. 2012 Jul;33(21):5423-30. doi: 10.1016/j.biomaterials.2012.03.055. Epub 2012 Apr 28.

Abstract

We genetically introduced the Fc-binding peptide (FcBP) into the loop of a self-assembled protein cage, ferritin, constituting four-fold symmetry at the surface to use it as a modular delivery nanoplatform. FcBP-presenting ferritin (FcBP-ferritin) formed very stable non-covalent complexes with both human and rabbit IgGs through the simple molecular recognition between the Fc region of the antibodies and the Fc-binding peptide clusters inserted onto the surface of FcBP-ferritin. This approach realized orientation-controlled display of antibodies on the surfaces of the protein cages simply by mixing without any complicated chemical conjugation. Using trastuzumab, a human anti-HER2 antibody used to treat patients with breast cancer, and a rabbit antibody to folate receptor, along with fluorescently labeled FcBP-ferritin, we demonstrated the specific binding of these complexes to breast cancer cells and folate receptor over-expressing cells, respectively, by fluorescent cell imaging. FcBP-ferritin may be potentially used as modular nanoplatforms for active targeted delivery vehicles or molecular imaging probes with a series of antibodies on demand.

摘要

我们将 Fc 结合肽(FcBP)基因引入到自组装蛋白笼的环中,在表面形成四重对称结构,将其用作模块化递药纳米平台。FcBP 呈现的铁蛋白(FcBP-铁蛋白)通过抗体 Fc 区域与插入到 FcBP-铁蛋白表面的 Fc 结合肽簇之间的简单分子识别,与人和兔 IgG 形成非常稳定的非共价复合物。这种方法通过简单的混合而无需任何复杂的化学偶联,实现了抗体在蛋白笼表面的定向控制展示。使用曲妥珠单抗(一种用于治疗乳腺癌患者的人抗 HER2 抗体)和兔抗叶酸受体抗体,以及荧光标记的 FcBP-铁蛋白,我们通过荧光细胞成像分别证明了这些复合物与乳腺癌细胞和叶酸受体过表达细胞的特异性结合。FcBP-铁蛋白可用作具有一系列按需抗体的主动靶向递药载体或分子成像探针的模块化纳米平台。

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