Melittin 类似物 p5RHH 可提高重组腺相关病毒的转导效率

IF 4.2 2区 医学 Q1 INTEGRATIVE & COMPLEMENTARY MEDICINE
Jing-shun Meng , Yun He , Heng-bin Yang , Li-ping Zhou , Si-yuan Wang , Xi-lin Feng , Omar Yahya Al-shargi , Xiao-min Yu , Li-qing Zhu , Chang-quan Ling
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引用次数: 0

摘要

目的 为支持有效的基因递送系统,开发了美利汀及其衍生物。它们促进内体释放的能力增强了基于纳米颗粒的基因治疗的传递。然而,其在病毒载体方面的潜在应用尚未得到广泛关注。因此,我们希望通过美利汀类似物优化 rAAV 载体,以提高 rAAV 在肝癌细胞中的转导效率,并探索美利汀类似物对 rAAV 的作用机制。对这些携带 gfp 或 fluc 基因的载体进行了定量聚合酶链反应检测,并在人胚肾 293(HEK293T)细胞中进行了转导检测,以研究载体生产和基因递送的效率。此外,还通过体外转导不同的培养细胞和体内尾静脉注射 C57BL/6 小鼠,检验了特定 p5RHH-rAAV 载体传递基因的能力。最后,通过使用 rAAV2 细胞内生命周期各阶段的药理抑制剂,探讨了载体介导转导机制的复杂细节。其中,CMA-3、p5RHH 和 aAR3 能显著抑制 rAAV2 载体粗裂解物的转导。p5RHH-rAAV2 载体不仅能有效地转导具有 rAAV 活性的细胞系,还能有效地转导以前被认为对 rAAV 具有抗性的细胞系。从机理上讲,巴佛洛霉素 A1(一种液泡内质体酸化抑制剂)完全抑制了 p5RHH-rAAV2 载体介导的转基因表达。最重要的是,p5RHH-rAAV8 载体还增加了 C57BL/6 小鼠体内的肝转导。我们的研究大大拓宽了美乐汀在病毒载体介导的基因递送中的药理前景:Meng JS, He Y, Yang HB, Zhou LP, Wang SY, Feng XL, Al-shargi OY, Yu XM, Zhu LQ, Ling CQ.美利汀类似物p5RHH可提高重组腺相关病毒的转导效率J Integr Med.2024; Epub ahead of print.
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Melittin analog p5RHH enhances recombinant adeno-associated virus transduction efficiency

Objective

Melittin and its derivative have been developed to support effective gene delivery systems. Their ability to facilitate endosomal release enhances the delivery of nanoparticle-based gene therapy. Nevertheless, its potential application in the context of viral vectors has not received much attention. Therefore, we would like to optimize the rAAV vector by Melittin analog to improve the transduction efficiency of rAAV in liver cancer cells and explore the mechanism of Melittin analog on rAAV.

Methods

Various melittin-derived peptides were inserted into loop VIII of the capsid protein in recombinant adeno-associated virus vectors. These vectors carrying either gfp or fluc genes were subjected to quantitative polymerase chain reaction assays and transduction assays in human embryonic kidney 293 (HEK293T) cells to investigate the efficiency of vector production and gene delivery. In addition, the ability of a specific p5RHH-rAAV vector to deliver genes was examined through in vitro transduction of different cultured cells and in vivo tail vein administration to C57BL/6 mice. Finally, the intricate details of the vector-mediated transduction mechanisms were explored by using pharmacological inhibitors of every stage of the rAAV2 intracellular life cycle.

Results

A total of 76 melittin-related peptides were identified from existing literature. Among them, CMA-3, p5RHH and aAR3 were found to significantly inhibit transduction of rAAV2 vector crude lysate. The p5RHH-rAAV2 vectors efficiently transduced not only rAAV-potent cell lines but also cell lines previously considered resistant to rAAV. Mechanistically, bafilomycin A1, a vacuolar endosome acidification inhibitor, completely inhibited the transgene expression mediated by the p5RHH-rAAV2 vectors. Most importantly, p5RHH-rAAV8 vectors also increased hepatic transduction in vivo in C57BL/6 mice.

Conclusion

The incorporation of melittin analogs into the rAAV capsids results in a significant improvement in rAAV-mediated transgene expression. While further modifications remain an area of interest, our studies have substantially broadened the pharmacological prospects of melittin in the context of viral vector-mediated gene delivery.

Please cite this article as: Meng J, He Y, Yang H, Zhou L, Wang S, Feng X, Al-shargi OY, Yu X, Zhu L, Ling, C. Melittin analog p5RHH enhances recombinant adeno-associated virus transduction efficiency. J Integr Med. 2024; 22(1): 72–82.

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来源期刊
Journal of Integrative Medicine-Jim
Journal of Integrative Medicine-Jim Medicine-Complementary and Alternative Medicine
CiteScore
9.20
自引率
4.20%
发文量
3319
期刊介绍: The predecessor of JIM is the Journal of Chinese Integrative Medicine (Zhong Xi Yi Jie He Xue Bao). With this new, English-language publication, we are committed to make JIM an international platform for publishing high-quality papers on complementary and alternative medicine (CAM) and an open forum in which the different professions and international scholarly communities can exchange views, share research and their clinical experience, discuss CAM education, and confer about issues and problems in our various disciplines and in CAM as a whole in order to promote integrative medicine. JIM is indexed/abstracted in: MEDLINE/PubMed, ScienceDirect, Emerging Sources Citation Index (ESCI), Scopus, Embase, Chemical Abstracts (CA), CAB Abstracts, EBSCO, WPRIM, JST China, Chinese Science Citation Database (CSCD), and China National Knowledge Infrastructure (CNKI). JIM Editorial Office uses ThomsonReuters ScholarOne Manuscripts as submitting and review system (submission link: http://mc03.manuscriptcentral.com/jcim-en). JIM is published bimonthly. Manuscripts submitted to JIM should be written in English. Article types include but are not limited to randomized controlled and pragmatic trials, translational and patient-centered effectiveness outcome studies, case series and reports, clinical trial protocols, preclinical and basic science studies, systematic reviews and meta-analyses, papers on methodology and CAM history or education, conference proceedings, editorials, commentaries, short communications, book reviews, and letters to the editor. Our purpose is to publish a prestigious international journal for studies in integrative medicine. To achieve this aim, we seek to publish high-quality papers on any aspects of integrative medicine, such as acupuncture and traditional Chinese medicine, Ayurveda medicine, herbal medicine, homeopathy, nutrition, chiropractic, mind-body medicine, taichi, qigong, meditation, and any other modalities of CAM; our commitment to international scope ensures that research and progress from all regions of the world are widely covered. These ensure that articles published in JIM have the maximum exposure to the international scholarly community. JIM can help its authors let their papers reach the widest possible range of readers, and let all those who share an interest in their research field be concerned with their study.
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