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一种基于树枝状聚合物的纳米载体,其与寡肽/适配体共轭,用于双靶点递送至骨骼。

An oligopeptide/aptamer-conjugated dendrimer-based nanocarrier for dual-targeting delivery to bone.

作者信息

Ren Mingxing, Li Yuzhou, Zhang He, Li Lingjie, He Ping, Ji Ping, Yang Sheng

机构信息

College of Stomatology, Chongqing Medical University, 426 Songshibei Road, Yubei District, Chongqing, 401147, China.

出版信息

J Mater Chem B. 2021 Mar 28;9(12):2831-2844. doi: 10.1039/d0tb02926b. Epub 2021 Mar 11.

DOI:10.1039/d0tb02926b
PMID:33704322
Abstract

Bone targeting is one of the most potentially valuable therapeutic methods for medically treating bone diseases, such as osteoarthritis, osteoporosis, nonunion bone defects, bone cancer, and myeloma-related bone disease, but its efficacy remains a challenge due to unfavorable bone biodistribution, off-target effects, and the lack of cell specificity. To address these problems, we synthesized a new dual-targeting nanocarrier for delivery to bone by covalently modifying the G4.0 PAMAM dendrimer with the C11 peptide and the CH6 aptamer (CH6-PAMAM-C11). The molecular structure was confirmed using H-NMR and FT-IR spectroscopy. CLSM results showed that the novel nanocarrier could successfully accumulate in the targeted cells, mineralized areas and tissues. DLS and TEM demonstrated that CH6-PAMAM-C11 was approximately 40-50 nm in diameter. In vitro targeting experiments confirmed that the C11 ligand had a high affinity for HAP, while the CH6 aptamer had a high affinity for osteoblasts. The in vivo biodistribution analysis showed that CH6-PAMAM-C11 could rapidly accumulate in bone within 4 h and 12 h and then deliver drugs to sites of osteoblast activity. The components of CH6-PAMAM-C11 were well excreted via the kidneys. The accumulation of many more CH6-PAMAM-C11 dual-targeting nanocarriers than single-targeting nanocarriers was observed in the periosteal layer of the rat skull, along with aggregation at sites of osteoblast activity. All of these results indicate that CH6-PAMAM-C11 may be a promising nanocarrier for the delivery of drugs to bone, particularly for the treatment of osteoporosis, and our research strategy may serve as a reference for research in targeted drug, small molecule drug and nucleic acid delivery.

摘要

骨靶向是医学治疗骨疾病(如骨关节炎、骨质疏松症、骨不连缺损、骨癌和骨髓瘤相关骨病)最具潜在价值的治疗方法之一,但由于不良的骨生物分布、脱靶效应和缺乏细胞特异性,其疗效仍然是一个挑战。为了解决这些问题,我们通过用C11肽和CH6适体(CH6-PAMAM-C11)共价修饰G4.0 PAMAM树枝状大分子,合成了一种用于递送至骨的新型双靶向纳米载体。使用H-NMR和FT-IR光谱确认了分子结构。CLSM结果表明,新型纳米载体能够成功地在靶向细胞、矿化区域和组织中积累。DLS和TEM表明CH6-PAMAM-C11的直径约为40-50nm。体外靶向实验证实,C11配体对HAP具有高亲和力,而CH6适体对成骨细胞具有高亲和力。体内生物分布分析表明,CH6-PAMAM-C11可在4小时和12小时内迅速在骨中积累,然后将药物递送至成骨细胞活性部位。CH6-PAMAM-C11的成分通过肾脏良好地排泄。在大鼠颅骨的骨膜层中观察到,与单靶向纳米载体相比,更多的CH6-PAMAM-C11双靶向纳米载体积累,同时在成骨细胞活性部位聚集。所有这些结果表明,CH6-PAMAM-C11可能是一种有前途的用于向骨递送药物的纳米载体,特别是用于治疗骨质疏松症,并且我们的研究策略可为靶向药物、小分子药物和核酸递送的研究提供参考。

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