纳米载体用于包载生物活性多肽的研究进展

doi:10.3969/j.issn.0258-8021.2023.02.013

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摘要多肽药物因其适应症广、安全性高且疗效显著,已广泛应用于肿瘤、肝炎、糖尿病、艾滋病等疾病的预防、诊断和治疗。但是,天然多肽进入人体后易被迅速降解并通过血液循环被迅速清除,安全递送是其发挥功效的基础。通过物理包埋、化学键合等手段合成基于多肽的纳米药物系统已解决这一问题的重要手段,具有生物安全性高,生物相容性好,易于修饰等特点,相关的开发研究正逐渐成为热点。综述多肽纳米给药系统的设计进展,总结抗菌肽、抗肿瘤肽、抗炎肽和肽疫苗等用于纳米药物递送的应用成果,展望未来生物活性多肽的临床应用前景,为当前构建负载多肽的纳米药物递送系统的研发提供有益建议。

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	郑珊珊
	蔡悦
	龚瑜贝
	洪煜璐
	孙漩嵘

关键词 ：生物活性多肽, 生物学功能, 构建, 纳米颗粒, 药物递送

Abstract：At present, due to wide indications, high safety and remarkable efficacy, peptide drugs have been widely used in the prevention, diagnosis and treatment of tumors, hepatitis, diabetes, AIDS and many other diseases. However, natural peptides are easy to be degraded when entering biological systems and can be quickly removed through the blood circulation. Thus, peptide-based nanomedicine systems, which are fabricated by physical encapsulation and chemical conjugation, have become a hotspot for researchers to construct the novel and intelligent drug delivery systems, because of high biological safety, good biocompatibility, and easy modification. Herein, we firstly described the common biological properties of bioactive peptides, such as antibacterial, antiviral, and antitumor effects, and then summarized the research on the construction of nanomedicine for drug delivery based on the bioactive peptides. Finally, we provided perspectives on the development of peptide-based nanomedicine which shows considerably promising future in the drug delivery.

Key words： therapeutic peptides biological properties construction nanomedicine drug delivery

收稿日期: 2021-09-21

PACS:

R318

基金资助:国家自然科学基金(22075247);浙江省基础公益研究计划(LGF21C100001)

通讯作者: ^*E-mail: sunxr@zjut.edu.cn

引用本文:

郑珊珊, 蔡悦, 龚瑜贝, 洪煜璐, 孙漩嵘. 纳米载体用于包载生物活性多肽的研究进展[J]. 中国生物医学工程学报, 2023, 42(2): 242-251.
Zheng Shanshan, Cai Yue, Gong Yubei, Hong Yulu, Sun Xuanrong. Research Progress onTherapeutic Peptides Loaded with Nanocarriers. Chinese Journal of Biomedical Engineering, 2023, 42(2): 242-251.

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http://cjbme.csbme.org/CN/10.3969/j.issn.0258-8021.2023.02.013 或 http://cjbme.csbme.org/CN/Y2023/V42/I2/242

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