首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >Rituximab conjugated iron oxide nanoparticles for targeted imaging and enhanced treatment against CD20-positive lymphoma
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Rituximab conjugated iron oxide nanoparticles for targeted imaging and enhanced treatment against CD20-positive lymphoma

机译:Rituximab缀合的氧化铁纳米粒子用于靶向成像和增强治疗CD20阳性淋巴瘤

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摘要

Since its launch in 1997, rituximab (RTX) has extensively improved the treatment of CD20-positive follicular and diffuse large B cell non-Hodgkin lymphoma (NHL). The application of RTX is limited usually by the failed therapy because of resistance. Iron oxide nanomaterials have been explored for cancer detection and treatment in recent years. In this study, a multivalent nanoprobe comprising one Fe3O4 nanoparticle and several RTX antibodies was constructed for the targeted imaging and enhanced treatment of NHL. Poly(ethylene glycol) (PEG)-coated Fe3O4 nanoparticles were fabricated via a thermal decomposition method and ligand exchange. RTX was conjugated onto the surface of the Fe3O4-PEG nanoparticles to form Fe3O4-PEG-nAb (n = 2, 5 or 8) multivalent nanoprobes. These multivalent nanoprobes, with a core size of approximately 11 nm and a hydrodynamic diameter of about 22 nm, showed colloidal stability in buffer solution. The r2 relaxation rate of Fe3O4-PEG-nAb was similar to that of Fe3O4-PEG (309 +/- 3.08 mM(-1) s(-1)). The specificity of nanoprobes for CD20-positive Raji cells was assessed on a clinical magnetic resonance imaging scanner. The receptor binding site of one multivalent nanoprobe was more than that of one RTX, exhibiting valence-dependent induction of Raji cell apoptosis, and this effect could be enhanced by complement activation from blood serum added. A similar activity was observed in vivo in a NHL xenograft model. The multivalent nanoprobe treatment significantly reduced tumor burden and enhanced survival in comparison to the RTX group. Our studies demonstrate that the appropriate design and preparation of anticancer antibody-nanoparticle conjugates enable the generation of improved anticancer nanomedicines and could thus provide an efficient cancer theranostic strategy.
机译:自1997年推出以来,Rituximab(RTX)已广泛改善CD20阳性滤泡和弥漫性大B细胞非霍奇金淋巴瘤(NHL)的治疗。 RTX的应用通常是由于由于阻力而失败的治疗。近年来探讨了氧化铁纳米材料用于癌症检测和治疗。在该研究中,构建了一种包含一个Fe3O4纳米颗粒和几种RTX抗体的多价纳米孔用于靶向成像和增强NHL的治疗。聚(乙二醇)(PEG) - 涂覆的Fe3O4纳米颗粒通过热分解方法和配体交换制备。将RTX缀合到Fe3O4-PEG纳米颗粒的表面上,形成Fe3O4-PEG-Nab(n = 2,5或8)多价纳米体。这些多价纳米素,核心尺寸约为11nm和液动力直径为约22nm,在缓冲溶液中显示出胶体稳定性。 Fe3O4-PEG-nab的R2弛豫率类似于Fe3O4-PEG(309 +/- 3.08mm(-1)S(-1))。在临床磁共振成像扫描仪上评估CD20阳性Raji细胞的纳米素物的特异性。一种多价纳米骨骨的受体结合位点大于RTX的受体结合位点,表现出Raji细胞凋亡的价依赖性诱导,并且通过加入的血清血清的补体激活可以提高这种效果。在NHL异种移植模型中在体内观察到类似的活性。多价纳米骨藻治疗与RTX组相比,肿瘤负荷显着降低,增强存活率。我们的研究表明,抗癌抗体 - 纳米粒子缀合物的适当设计和制备使得改善的抗癌纳米海内西林,因此可以提供有效的癌症治疗癌症策略。

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    Nanjing Univ Chinese Med Jiangsu Prov Hosp Chinese Med Dept Radiol Affiliated Hosp Nanjing 210029 Peoples R China;

    Southeast Univ State Key Lab Bioelect Jiangsu Key Lab Biomat &

    Devices Sch Biol Sci &

    Med Engn Nanjing 210096 Peoples R China;

    Southeast Univ Zhongda Hosp Informat Ctr Nanjing 210009 Peoples R China;

    Southeast Univ State Key Lab Bioelect Jiangsu Key Lab Biomat &

    Devices Sch Biol Sci &

    Med Engn Nanjing 210096 Peoples R China;

    Nanjing Med Univ Jiangsu Prov Res Inst Clin Med Affiliated Hosp 1 Nanjing 210009 Peoples R China;

    Southeast Univ State Key Lab Bioelect Jiangsu Key Lab Biomat &

    Devices Sch Biol Sci &

    Med Engn Nanjing 210096 Peoples R China;

    Southeast Univ Med Sch Jiangsu Key Lab Mol &

    Funct Imaging Nanjing 210009 Peoples R China;

    Nanjing Univ Chinese Med Jiangsu Prov Hosp Chinese Med Dept Radiol Affiliated Hosp Nanjing 210029 Peoples R China;

    Southeast Univ State Key Lab Bioelect Jiangsu Key Lab Biomat &

    Devices Sch Biol Sci &

    Med Engn Nanjing 210096 Peoples R China;

    Southeast Univ State Key Lab Bioelect Jiangsu Key Lab Biomat &

    Devices Sch Biol Sci &

    Med Engn Nanjing 210096 Peoples R China;

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  • 正文语种 eng
  • 中图分类 分析化学;
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