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Brain tumor tandem targeting using a combination of monoclonal antibodies attached to biopoly(β-L-malic acid)

机译:使用与生物聚(β-L-苹果酸)连接的单克隆抗体的组合靶向脑肿瘤

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摘要

Tumor-specific targeting using achievements of nanotechnology is a mainstay of increasing efficacy of anti-tumor drugs. To improve drug targeting we covalently conjugated for the first time two different monoclonal antibodies, an anti-mouse transferrin receptor antibody and a mouse autoimmune anti-nucleosome antibody 2C5, onto the drug delivery nanoplatform, poly(β-L-malic acid). The active anti-tumor drug components attached to the same carrier molecule were antisense oligonucleotides to vascular protein laminin-8. The resulting drug, a new Polycefin variant, was administered intravenously into glioma-bearing xenogeneic animals. The drug delivery system was targeted across mouse endothelial system by the anti-mouse transferring receptor antibody and to the tumor cell surface by the anti-nucleosome antibody 2C5. The targeting efficacies of the Polycefin variants bearing either two antibodies or each single antibody were compared in vitro and in vivo. ELISA confirmed the co-existence of two antibodies on the same nanoplatform molecule and their functional activities. Fluorescence imaging analysis after 24 h of intravenous injection demonstrated significantly higher tumor accumulation of Polycefin variants with the tandem configuration of antibodies than with single antibodies. The results suggest improved efficacy for tandem configuration of antibodies than for single configurations carried by a drug delivery vehicle.
机译:利用纳米技术取得的肿瘤特异性靶向是提高抗肿瘤药物疗效的主要手段。为了提高药物靶向性,我们首次将两种不同的单克隆抗体(一种抗小鼠转铁蛋白受体抗体)和一种小鼠自身免疫性抗核小体抗体2C5共价偶联到了药物递送纳米平台聚(β-L-苹果酸)上。附着在同一载体分子上的活性抗肿瘤药物成分是血管蛋白层粘连蛋白8的反义寡核苷酸。将得到的药物,一种新的Polycefin变体,静脉注射给具有神经胶质瘤的异种动物。通过抗小鼠转移受体抗体将药物递送系统靶向整个小鼠内皮系统,并通过抗核小体抗体2C5靶向肿瘤细胞表面。在体外和体内比较了带有两种抗体或每种单一抗体的Polycefin变体的靶向效力。 ELISA证实了同一纳米平台分子上两种抗体的共存及其功能活性。静脉注射24小时后的荧光成像分析表明,具有串联抗体配置的Polycefin变体在肿瘤中的蓄积明显高于单一抗体。结果表明,与药物递送载体所携带的单一构型相比,抗体的串联构型具有更高的功效。

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