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抗体递送平台的细胞内转运、细胞质生物利用度和靶标操作的示踪。

Demonstration of intracellular trafficking, cytosolic bioavailability, and target manipulation of an antibody delivery platform.

机构信息

School of Chemical & Biomolecular Engineering and Petit Institute for Bioengineering and Bioscience, Georgia Institute of Technology, Atlanta, GA, United States.

School of Chemical & Biomolecular Engineering and Petit Institute for Bioengineering and Bioscience, Georgia Institute of Technology, Atlanta, GA, United States.

出版信息

Nanomedicine. 2021 Feb;32:102315. doi: 10.1016/j.nano.2020.102315. Epub 2020 Oct 13.

Abstract

Intracellular antibody delivery into live cells has significant implications for research and therapeutic applications. However, many delivery systems lack potency due to low uptake and/or endosomal entrapment and understanding of intracellular delivery processes is lacking. Herein, we studied the cellular uptake, intracellular trafficking and targeting of antibodies using our previously developed Hex antibody nanocarrier. We demonstrated Hex-antibodies were internalized through multiple endocytic routes into lysosomes and provide evidence of endo/lysosomal disruption and Hex-antibody release to the cytosol. Cytosolic antibodies retained their bioactivity for at least 24 h. Functional effect of Hex delivered anti-STAT3 antibodies was evidenced by inhibition of nuclear translocation of cytosolic transcription factor STAT3. This study has generated understanding of key steps in the Hex intracellular antibody delivery system and will facilitate the development of effective cytosolic antibody delivery and applications in both the therapeutic and research domains.

摘要

细胞内抗体递送至活细胞在研究和治疗应用方面具有重要意义。然而,由于摄取率低和/或内体捕获,许多递药系统效力不足,并且对细胞内递药过程的了解也很有限。在此,我们使用先前开发的六聚体抗体纳米载体研究了抗体的细胞摄取、细胞内转运和靶向作用。我们证明六聚体抗体通过多种内吞途径被内化到溶酶体中,并提供了内体/溶酶体破坏和六聚体抗体释放到细胞质的证据。细胞质中的抗体至少在 24 小时内保持其生物活性。递送至细胞质中的抗 STAT3 抗体的功能作用通过抑制细胞质转录因子 STAT3 的核易位得到证实。这项研究深入了解了六聚体细胞内抗体递药系统的关键步骤,将有助于开发有效的细胞质抗体递药系统,并在治疗和研究领域得到广泛应用。

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