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Near-infrared light photocontrolled targeting, bioimaging, and chemotherapy with caged upconversion nanoparticles in vitro and in vivo

机译:笼状上转换纳米粒子在体外和体内的近红外光控靶向,生物成像和化学疗法

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The major challenge in current chemotherapy is to increase local effective therapeutic concentration of drugs as well as to minimize toxicity and side effects for patients. The targeted delivery of drugs to their desired site of action in a controlled manner plays an essential role in the development of drug formulations. A photocage refers to a caged molecule rendered biologically inert by a photolabile protecting group. Molecules are illuminated with light to liberate the caged group and then become active forms. In this study, we formulate upconversion nanoparticles (UCNPs) as the NIR-triggered targeting and drug delivery vehicles that successfully deliver in vitro and in vivo for near-infrared light photocontrolled targeting, bioimaging, and chemotherapy. It is noted that there has been no report on the systemic administration UCNP-based drug delivery agents for evaluation of bioimaging and chemotherapy. To achieve phototargeting, the tumor-homing agent (i.e., folic acid) has been constructed as a photoresponsive molecule. For the chemotherapeutic effect, the antitumor drug doxorubicin is thiolated on the surface of UCNPs, forming a disulfide bond that can be cleaved by lysosomal enzymes within the cells. The caged UNCPs can serve as a platform for the improvement of selective targeting and possible reduction of adverse side effects from chemotherapy.
机译:当前化学疗法的主要挑战是增加药物的局部有效治疗浓度以及最小化对患者的毒性和副作用。以受控方式将药物靶向递送至其期望的作用部位在药物制剂的开发中起重要作用。光笼是指被光不稳定的保护基团变成生物学惰性的笼状分子。用光照射分子以释放笼中的基团,然后变成活性形式。在这项研究中,我们将上转换纳米粒子(UCNPs)配制为NIR触发的靶向和药物递送载体,可成功地在体内和体外递送近红外光控靶向,生物成像和化学疗法。要指出的是,还没有关于基于全身给药基于UCNP的药物递送剂用于评估生物成像和化学疗法的报道。为了实现光靶向,已经将肿瘤归巢剂(即叶酸)构建为光响应分子。对于化学治疗作用,抗肿瘤药物阿霉素在UCNPs的表面上被硫醇化,形成二硫键,可被细胞内的溶酶体酶裂解。关在笼中的UNCP可以作为改善选择性靶向和可能减少化疗带来的不良副作用的平台。

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