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Tumor target amplification: Implications for nano drug delivery systems

机译:肿瘤靶扩增:对纳米药物递送系统的影响

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摘要

Tumor cells overexpress surface markers which are absent from normal cells. These tumor-restricted antigenic signatures are a fundamental basis for distinguishing on-target from off-target cells for ligand-directed targeting of cancer cells. Unfortunately, tumor heterogeneity impedes the establishment of a solid expression pattern for a given target marker, leading to drastic changes in quality (availability) and quantity (number) of the target. Consequently, a subset of cancer cells remains untargeted during the course of treatment, which subsequently promotes drug-resistance and cancer relapse. Since target inefficiency is only problematic for cancer treatment and not for treatment of other pathological conditions such as viral/bacterial infections, target amplification or the generation of novel targets is key to providing eligible antigenic markers for effective targeted therapy. This review summarizes the limitations of current ligand-directed targeting strategies and provides a comprehensive overview of tumor target amplification strategies, including self-amplifying systems, dual targeting, artificial markers and peptide modification. We also discuss the therapeutic and diagnostic potential of these approaches, the underlying mechanism(s) and established methodologies, mostly in the context of different nanodelivery systems, to facilitate more effective ligand-directed cancer cell monitoring and targeting.
机译:肿瘤细胞过表达表面标志物不存在于正常细胞。这些肿瘤限制的抗原性签名是区分靶细胞的基础基础,用于癌细胞的配体定向靶向靶细胞。不幸的是,肿瘤异质性阻碍了给定靶标记的固体表达模式,导致靶标的质量(可用性)和数量(数量)的变化。因此,在治疗过程中,癌细胞的子集仍未明确,随后促进耐药性和癌症复发。由于目标低效率仅为癌症治疗问题而不是治疗其他病态条件,例如病毒/细菌感染,靶扩增或新靶的产生是为有效靶向治疗提供资格的抗原标志物的关键。本综述总结了当前配体定向的靶向策略的局限性,并提供了肿瘤目标扩增策略的全面概述,包括自我放大系统,双重靶向,人工标志物和肽改性。我们还讨论了这些方法的治疗和诊断潜力,潜在的机制和建立的方法,主要是在不同纳米交货系统的背景下,以促进更有效的配体定向的癌细胞监测和靶向。

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