首页> 美国卫生研究院文献>Acta Pharmaceutica Sinica. B >Cathepsin B-responsive and gadolinium-labeled branched glycopolymer-PTX conjugate-derived nanotheranostics for cancer treatment
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Cathepsin B-responsive and gadolinium-labeled branched glycopolymer-PTX conjugate-derived nanotheranostics for cancer treatment

机译:组织蛋白酶B响应和钆标记的支链甘油聚合物-PTX缀合物衍生的纳米移植物用于癌症治疗方法

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摘要

Multi-modal therapeutics are emerging for simultaneous diagnosis and treatment of cancer. Polymeric carriers are often employed for loading multiple drugs due to their versatility and controlled release of these drugs in response to a tumor specific microenvironment. A theranostic nanomedicine was designed and prepared by complexing a small gadolinium chelate, conjugating a chemotherapeutic drug PTX through a cathepsin B-responsive linker and covalently bonding a fluorescent probe pheophorbide a (Ppa) with a branched glycopolymer. The branched prodrug-based nanosystem was degradable in the tumor microenvironment with overexpressed cathepsin B, and PTX was simultaneously released to exert its therapeutic effect. The theranostic nanomedicine, branched glycopolymer-PTX-DOTA-Gd, had an extended circulation time, enhanced accumulation in tumors, and excellent biocompatibility with significantly reduced gadolinium ion (Gd3+) retention after 96 h post-injection. Enhanced imaging contrast up to 24 h post-injection and excellent antitumor efficacy with a tumor inhibition rate more than 90% were achieved from glycopolymer-PTX-DOTA-Gd without obvious systematic toxicity. This branched polymeric prodrug-based nanomedicine is very promising for safe and effective diagnosis and treatment of cancer.
机译:多种模式治疗癌症同时诊断和治疗。聚合物载体通常用于负载多种药物,由于它们的多功能性和控制这些药物的响应于肿瘤特异性微环境而受到控制释放。通过络合小钆螯合物,通过组织蛋白酶B响应性接头将化学治疗药物PTX缀合并与支链甘油聚合物共价键合,通过组织蛋白酶B响应螯合物,与支化甘油聚合物共价键合。基于支链的前药基纳米系统在肿瘤微环境中可降解,其具有过表达的组织蛋白酶B,同时释放PTX以施加其治疗效果。纳米胺胺,支化甘油聚合物-PTX-DOTA-GD具有延长的循环时间,肿瘤增强,并在注射后96小时后具有显着降低的钆离子(GD3 +)保留的优异生物相容性。增强的成像对比度为24小时,从甘氨酸-PTX-DOTA-GD达到90%以上的肿瘤抑制率的注射后和优异的抗肿瘤功效,而不是明显的系统毒性。该支化的聚合物前药基纳米卫生型对于癌症的安全有效诊断和治疗非常有前途。

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