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用于天然抗体胞质递送的细胞穿透性生物适配体:一种“即混即用”方法。

Cell-Permeant Bioadaptors for Cytosolic Delivery of Native Antibodies: A "Mix-and-Go" Approach.

作者信息

Du Shubo, Liew Si Si, Zhang Cheng-Wu, Du Wei, Lang Wenjie, Yao Cassandra C Y, Li Lin, Ge Jingyan, Yao Shao Q

机构信息

Department of Chemistry, National University of Singapore, Singapore 117543, Singapore.

Shaanxi Institute of Flexible Electronics (SIFE) & Xi'an Key Laboratory of Biomedical Materials & Engineering, Northwestern Polytechnical University (NPU), Xi'an 710072, China.

出版信息

ACS Cent Sci. 2020 Dec 23;6(12):2362-2376. doi: 10.1021/acscentsci.0c01379. Epub 2020 Nov 27.

Abstract

Antibodies are powerful tools that may potentially find wide applications in live-cell bioimaging, disease diagnostics, and therapeutics. Their practical applications have however remained limited thus far, owing to their inability to cross the cell membrane. Existing approaches for cytosolic delivery of functional antibodies are available, but they are constantly plagued by the need for chemical/genetic modifications, low delivery efficiency, and severe endolysosomal trapping. Consequently, it is of paramount importance to develop new strategies capable of highly efficient cytosolic delivery of native antibodies with immediate bioavailability. Herein, we report a modification-free, convenient "mix-and-go" strategy for the cytosolic delivery of native antibodies to different live mammalian cells efficiently, with minimal endolysosomal trapping and immediate bioavailability. By simply mixing a cell-permeant bioadaptor (derived from protein A or TRIM21) with a commercially available off-the-shelf antibody, the resulting noncovalent complex could be immediately used for intracellular delivery of native antibodies needed in subsequent cytosolic target engagement. The versatility of this approach was successfully illustrated in a number of applications, including antibody-based, live-cell imaging of the endogenous protein glutathionylation to detect oxidative cell stress, antibody-based activation of endogenous caspase-3, and inhibition of endogenous PTP1B activity, and finally TRIM21-mediated endogenous protein degradation for potential targeted therapy. Our results thus indicate this newly developed, "mix-and-go" antibody delivery method should have broad applications in chemical biology and future drug discovery.

摘要

抗体是强大的工具,在活细胞生物成像、疾病诊断和治疗中可能有广泛应用。然而,由于其无法穿过细胞膜,其实际应用迄今仍很有限。现有的将功能性抗体递送至细胞质的方法是有的,但它们一直受到化学/基因修饰需求、低递送效率和严重的内溶酶体捕获的困扰。因此,开发能够高效地将天然抗体递送至细胞质且具有即时生物利用度的新策略至关重要。在此,我们报告了一种无需修饰、便捷的“混合即用”策略,可将天然抗体高效地递送至不同的活哺乳动物细胞的细胞质中,内溶酶体捕获最少且具有即时生物利用度。通过简单地将一种细胞穿透性生物适配体(源自蛋白A或TRIM21)与市售现成抗体混合,所形成的非共价复合物可立即用于随后细胞质靶点结合所需的天然抗体的细胞内递送。这种方法的多功能性在许多应用中得到了成功展示,包括基于抗体的对内源性蛋白质谷胱甘肽化进行活细胞成像以检测氧化细胞应激、基于抗体的激活内源性半胱天冬酶-3以及抑制内源性蛋白酪氨酸磷酸酶1B活性,最后是TRIM21介导的内源性蛋白质降解用于潜在的靶向治疗。因此我们结果表明,这种新开发的“混合即用”抗体递送方法在化学生物学和未来药物发现中应具有广泛应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f657/7760483/4259139313cb/oc0c01379_0001.jpg

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