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将羟基磷灰石纳米晶体与人免疫球蛋白 G 缀合用于纳米医学应用。

Conjugation of hydroxyapatite nanocrystals with human immunoglobulin G for nanomedical applications.

机构信息

Dipartimento di Scienze Mediche, Università del Piemonte Orientale A. Avogadro, Novara, Italy.

出版信息

Colloids Surf B Biointerfaces. 2012 Feb 1;90:1-7. doi: 10.1016/j.colsurfb.2011.09.033. Epub 2011 Sep 24.

DOI:10.1016/j.colsurfb.2011.09.033
PMID:22015181
Abstract

Inorganic nanosized drug carriers are a promising field in nanomedicine applied to cancer. Their conjugation with antibodies combines the properties of the nanoparticles themselves with the specific and selective recognition ability of the antibodies to antigens. Biomimetic carbonate-hydroxyapatite (HA) nanoparticles were synthesized and fully characterized; human IgGs, used as model antibodies, were coupled to these nanocrystals. The maximum loading amount, the interaction modelling, the preferential orientation and the secondary structure modifications were evaluated using theoretical models (Langmuir, Freundlich and Langmuir-Freundlich) spectroscopic (UV-Vis, Raman), calorimetric (TGA), and immunochemical techniques (ELISA, Western Blot). HA nanoparticles of about 30 nm adsorbed human IgGs, in a dose-dependent, saturable and stable manner with micromolar affinity and adsorption capability around 2.3 mg/m(2). Adsorption isotherm could be described by Langmuir-Freundlich model, and was due to both energetically homogeneous and heterogeneous binding sites on HA surface, mainly of electrostatic nature. Binding did not induce secondary structure modification of IgGs. A preferential IgG end-on orientation with the involvement of IgG Fc moiety in the adsorption seems most probable due to the steric hindrance of their Fab domains. Biomimetic HA nanocrystals are suitable substrates to produce nanoparticles which can be functionalized with antibodies for efficient targeted drug delivery to tumours.

摘要

无机纳米药物载体是纳米医学在癌症治疗方面很有前途的一个领域。它们与抗体的结合结合了纳米粒子本身的特性和抗体对抗原的特异性和选择性识别能力。仿生碳酸羟基磷灰石(HA)纳米粒子被合成并进行了全面的表征;人免疫球蛋白 G(IgG)被用作模型抗体,与这些纳米晶体偶联。使用理论模型(朗缪尔、弗伦德利希和朗缪尔-弗伦德利希)、光谱(紫外-可见、拉曼)、量热(TGA)和免疫化学技术(ELISA、Western Blot)评估了最大负载量、相互作用模型、优先取向和二级结构修饰。约 30nm 的 HA 纳米粒子以剂量依赖、饱和和稳定的方式吸附人 IgG,亲和力为微摩尔级,吸附能力约为 2.3mg/m2。吸附等温线可以用朗缪尔-弗伦德利希模型来描述,这是由于 HA 表面上存在能量均匀和不均匀的结合位点,主要是静电性质。结合不会引起 IgG 二级结构的修饰。由于其 Fab 结构域的空间位阻,IgG 可能以优先的末端取向与 IgG Fc 部分参与吸附,这似乎是最有可能的。仿生 HA 纳米晶体是合适的基底,可以将抗体功能化,用于高效靶向药物输送到肿瘤。

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