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抗体偶联药物:基于人铁蛋白的蛋白笼纳米颗粒包载顺铂靶向黑色素瘤

Antibody-drug conjugates: targeting melanoma with cisplatin encapsulated in protein-cage nanoparticles based on human ferritin.

机构信息

CNR - National Research Council of Italy, Institute of Molecular Biology and Pathology, Rome, Italy.

出版信息

Nanoscale. 2013 Dec 21;5(24):12278-85. doi: 10.1039/c3nr04268e.

Abstract

A novel antibody-drug conjugate (ADC) was synthesized incorporating ferritin-based nanoparticles. An average of three molecules of monoclonal antibody (mAb) Ep1 to the human melanoma-specific antigen CSPG4 were conjugated to a single ferritin cage encapsulating about 50 cisplatin molecules (HFt-Pt-Ep1). The HFt-Pt-Ep1 nanoparticle had an estimated molecular size of about 900 kD and 33 nm, and flow cytometry demonstrated specific binding to a CSPG4(+) melanoma cell line, but not to a CSPG4(-) breast carcinoma cell line. As compared to the cisplatin-containing ferritin nanoparticle alone (HFt-Pt), which inhibited thymidine incorporation more efficiently in breast carcinoma than melanoma cells, the mAb-derivatized HFt-Pt-Ep1 nanoparticle had a 25-fold preference for the latter. A similar preference for melanoma was observed upon systemic intravenous administration of HFt-Pt-Ep1 to nude mice xenotransplanted with pre-established, palpable melanoma and breast carcinoma tumors. Thus, we have been able to determine precise combinations and stoichiometric relationships between mAbs and nanoparticle protein cages, whereby the latter lose their tropism for ubiquitously distributed cellular receptors, and acquire instead remarkably lineage-selective binding. HFt-Pt-Ep1 is therefore an interesting model to improve the therapeutic index of antiblastic therapy in a tumor such as melanoma, which at its advanced stages is totally refractory to mono- and combination-chemotherapy.

摘要

一种新型抗体药物偶联物(ADC)被合成,其中包含基于铁蛋白的纳米颗粒。将平均三个分子的抗人类黑色素瘤特异性抗原 CSPG4 的单克隆抗体(mAb)Ep1 连接到单个铁蛋白笼上,该笼可封装约 50 个顺铂分子(HFt-Pt-Ep1)。HFt-Pt-Ep1 纳米颗粒的估计分子大小约为 900 kD 和 33 nm,流式细胞术表明其与 CSPG4(+)黑色素瘤细胞系特异性结合,但与 CSPG4(-)乳腺癌细胞系不结合。与仅含有顺铂的铁蛋白纳米颗粒(HFt-Pt)相比,后者更有效地抑制胸苷掺入乳腺癌细胞而非黑色素瘤细胞,mAb 衍生的 HFt-Pt-Ep1 纳米颗粒对后者的偏好性高 25 倍。当将 HFt-Pt-Ep1 静脉内系统给药给预先建立的可触及黑色素瘤和乳腺癌肿瘤的裸鼠异种移植时,观察到对黑色素瘤具有类似的偏好性。因此,我们已经能够确定 mAb 和纳米颗粒蛋白笼之间的精确组合和化学计量关系,其中后者失去对普遍分布的细胞受体的趋性,而获得显著的谱系选择性结合。因此,HFt-Pt-Ep1 是一个有趣的模型,可以提高在诸如黑色素瘤等肿瘤中的抗肿瘤治疗指数,在晚期阶段,黑色素瘤对单药和联合化疗完全耐药。

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