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Utilization of monoclonal antibody-targeted nanomaterials in the treatment of cancer

机译:靶向单克隆抗体的纳米材料在癌症治疗中的应用

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摘要

Due to their excellent specificity for a single epitope, monoclonal antibodies (mAbs) present a means of influencing the function of cells at the molecular level. In particular they show great promise in the treatment of cancer because they can inhibit cancer cell proliferation, tumor angiogenesis, invasiveness and malignant spread of cancerous cells. Many mAbs are in various stages of testing and 11 are currently marketed in the US or Europe for the treatment of cancers that express particular antigens such as human epidermal growth factor receptor-2, CD20, epidermal growth factor receptor and vascular endothelial growth factor. Strategies to conjugate mAbs to toxins, radioactive isotopes and chemotherapeutic drugs to improve efficacy are under intense investigation and numerous immunoconjugates have been studied in the clinical setting. However, the molecules have limitations, and so nanomaterials (NMs), which potentially offer more flexibility of design and functionality in providing platforms for binding of multiple therapeutic agents in a single structure, are being examined as an alternative. Studies utilizing mAb-targeted NMs have shown that they exhibit focused targeting, improved pharmacokinetics and improved “passive” drug delivery via leaky vasculature. Nevertheless, before they can be utilized to treat cancer, potential NM toxicity must be thoroughly investigated. Thus, rigorous testing of NM-mAb conjugates in both in vitro and in vivo systems is underway to determine how NM-mAb conjugates will interact with cells and tissues of the body. In this review, we discuss the broad range of nanomaterials that are under investigation as potential platforms for the presentation of mAbs either as single therapeutics or in combination with other drugs and their advantages and limitations in specifically targeting cancer.
机译:由于其对单个表位的出色特异性,单克隆抗体(mAbs)提供了一种在分子水平上影响细胞功能的手段。特别是它们在癌症的治疗中显示出巨大的希望,因为它们可以抑制癌细胞的增殖,肿瘤血管生成,癌细胞的侵袭性和恶性扩散。许多mAb处于不同的测试阶段,目前有11种在美国或欧洲销售,用于治疗表达特定抗原的癌症,例如人表皮生长因子受体2,CD20,表皮生长因子受体和血管内皮生长因子。将mAb与毒素,放射性同位素和化学治疗药物偶联以提高功效的策略正在深入研究中,并且在临床环境中已研究了许多免疫偶联物。但是,分子具有局限性,因此正在研究纳米材料(NMs)的替代方法,该材料可提供设计和功能上更多的灵活性,从而提供用于在单一结构中结合多种治疗剂的平台。利用针对mAb的NMs进行的研究表明,它们表现出针对性的靶向,改善的药代动力学和通过泄漏的脉管系统改善的“被动”药物递送。然而,在将其用于治疗癌症之前,必须彻底研究潜在的NM毒性。因此,正在进行在体外和体内系统中NM-mAb缀合物的严格测试,以确定NM-mAb缀合物将如何与身体的细胞和组织相互作用。在这篇综述中,我们讨论了广泛的纳米材料,这些纳米材料正在研究中,它们可作为单克隆抗体作为单一疗法或与其他药物联合使用的潜在平台,以及它们在特异性靶向癌症方面的优势和局限性。

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