Dual-aptamer-decorated reduction-activated dimeric-prodrug nanoparticles for broad-spectrum treatment of leukemia.

Shan Yang, Riming Wang, Mei Liu, Yanhong Lv, Hong Fu, Xiaochen Cao, Guogang Dong
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Abstract

Leukemia remains a fatal disease for most affected patients, and a simple and effective therapeutic strategy is urgently needed. Targeted delivery chemo-drugs to leukemia cells shows promise, but the diverse subtypes of leukemia make single-ligand nanomedicine often ineffective. Herein, a dual-aptamer decorated, reduction-responsive dimeric prodrug-based nanoparticle (NP), termed SXP-NPs, was developed using the two leukemia-specific aptamers Sgc8c and XQ-2d, a reduction-responsive podophyllotoxin (POD) dimeric prodrug, and DSPE-PEG2000. Because the receptors of XQ-2d (CD71) and Sgc8c (PTK7) are overexpressed in different subtypes of leukemia cells, SXP-NPs can broadly and selectively recognize these leukemia cells after intravenous administration, subsequently releasing POD in response to the intracellular high-reduction environment to kill the leukemia cells. In vitro experiments showed that these simple SXP-NPs can specifically bind to various leukemia cancer cells and kill them. In vivo experiments revealed that SXP-NPs can remarkably reduce spleen weight, decrease white blood cell counts, and extend overall survival in a preclinical leukemia animal model. The in vitro and in vivo validation demonstrated that SXP-NPs offer several advantages, including high drug-loading potential, broad-spectrum recognition of leukemia cells, reduced systemic toxicity, and enhanced therapeutic effects of the drug. Taken together, this study provides a simple and effective strategy for broad-spectrum leukemia therapy and highlights the clinical potential of SXP-NPs.

用于广谱治疗白血病的双aptamer-decorated-reducing-activated dimeric-pro-drug纳米粒子。
对于大多数患者来说,白血病仍然是一种致命疾病,因此迫切需要一种简单有效的治疗策略。向白血病细胞靶向输送化疗药物的前景看好,但由于白血病的亚型多样,单一配体的纳米药物往往效果不佳。在此,我们利用两种白血病特异性适配体 Sgc8c 和 XQ-2d、一种还原反应型 podophyllotoxin(POD)二聚体原药和 DSPE-PEG2000 开发了一种双适配体装饰、还原反应型二聚体原药纳米粒子(NP),称为 SXP-NPs。由于 XQ-2d(CD71)和 Sgc8c(PTK7)的受体在不同亚型的白血病细胞中过度表达,因此静脉注射 SXP-NPs 后可广泛并选择性地识别这些白血病细胞,然后在细胞内高还原环境下释放 POD,杀死白血病细胞。体外实验表明,这些简单的 SXP-NPs 可特异性地与各种白血病癌细胞结合并杀死它们。体内实验表明,在临床前白血病动物模型中,SXP-NPs 能显著减轻脾脏重量、降低白细胞计数并延长总生存期。体外和体内验证表明,SXP-NPs 具有多种优势,包括药物负载潜力大、可广谱识别白血病细胞、降低全身毒性和增强药物治疗效果。总之,这项研究为广谱白血病治疗提供了一种简单有效的策略,并凸显了 SXP-NPs 的临床潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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