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Assessing the in vivo targeting efficiency of multifunctional nanoconstructs bearing antibody-derived ligands

机译:评估带有抗体衍生配体的多功能纳米构建体的体内靶向效率

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A great challenge in nanodiagnostics is the identification of new strategies aimed to optimize the detection of primary breast cancer and metastases by the employment of target-specific nanodevices. At present, controversial proof has been provided on the actual importance of surface functionalization of nanoparticles to improve their in vivo localization at the tumor. In the present paper, we have designed and developed a set of multifunctional nanoprobes, modified with three different variants of a model antibody, that is, the humanized monocolonal antibody trastuzumab (TZ), able to selectively target the HER2 receptor in breast cancer cells. Assuming that nanoparticle accumulation in target cells is strictly related to their physicochemical properties, we performed a comparative study of internalization, trafficking, and metabolism in MCF7 cells of multifunctional nanoparticles (MNP) functionalized with TZ or with alternative lower molecular weight variants of the monoclonal antibody, such as the half-chain (HC) and scFv fragments (scFv). Hence, to estimate to what extent the structure of the surface bioligand affects the targeting efficiency of the nanoconjugate, three cognate nanoconstructs were designed, in which only the antibody form was differentiated while the nanoparticle core was maintained unvaried, consisting of an iron oxide spherical nanocrystal coated with an amphiphilic polymer shell. In vitro, in vivo, and ex vivo analyses of the targeting efficiency and of the intracellular fate of MNP-TZ, MNP-HC, and MNP-scFv suggested that the highly stable MNP-HC is the best candidate for application in breast cancer detection. Our results provided evidence that, in this case, active targeting plays an important role in determining the biological activity of the nanoconstruct.
机译:纳米诊断学中的一大挑战是确定新策略,这些策略旨在通过使用靶标特异性纳米器件来优化对原发性乳腺癌和转移瘤的检测。目前,关于纳米颗粒的表面功能化对于改善其在肿瘤中的体内定位的实际重要性的争议性证据已经提供。在本文中,我们设计和开发了一组多功能纳米探针,这些探针经模型抗体的三种不同变体修饰,即人源化单克隆抗体曲妥珠单抗(TZ),能够选择性靶向乳腺癌细胞中的HER2受体。假设纳米颗粒在靶细胞中的积累与它们的理化特性严格相关,我们进行了一项对TZF或单克隆抗体的其他较低分子量变体功能化的多功能纳米颗粒(MNP)MCF7细胞内在化,运输和代谢的比较研究。 ,例如半链(HC)和scFv片段(scFv)。因此,为了估计表面生物配体的结构在多大程度上影响纳米复合物的靶向效率,设计了三种同源的纳米结构,其中仅抗体形式被区分,而纳米颗粒核心保持不变,由氧化铁球形纳米晶体组成涂有两亲聚合物外壳。体外,体内和离体分析靶向性和MNP-TZ,MNP-HC和MNP-scFv的细胞内命运表明,高度稳定的MNP-HC是用于乳腺癌检测的最佳候选者。我们的结果提供了证据,在这种情况下,主动靶向在确定纳米结构的生物学活性中起着重要作用。

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