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通过代谢标记和点击化学的组合实现纳米颗粒的共价细胞表面偶联。

Covalent Cell Surface Conjugation of Nanoparticles by a Combination of Metabolic Labeling and Click Chemistry.

机构信息

Department of Pharmaceutics, Ghent University, Ghent, Belgium.

出版信息

Angew Chem Int Ed Engl. 2021 Mar 15;60(12):6320-6325. doi: 10.1002/anie.202015625. Epub 2021 Feb 17.

Abstract

Conjugation of nanoparticles (NP) to the surface of living cells is of interest in the context of exploiting the tissue homing properties of ex vivo engineered T cells for tumor-targeted delivery of drugs loaded into NP. Cell surface conjugation requires either a covalent or non-covalent reaction. Non-covalent conjugation with ligand-decorated NP (LNP) is challenging and involves a dynamic equilibrium between the bound and unbound state. Covalent NP conjugation results in a permanently bound state of NP, but the current routes for cell surface conjugation face slow reaction kinetics and random conjugation to proteins in the glycocalyx. To address the unmet need for alternative bioorthogonal strategies that allow for efficient covalent cell surface conjugation, we developed a 2-step click conjugation sequence in which cells are first metabolically labeled with azides followed by reaction with sulfo-6-methyl-tetrazine-dibenzyl cyclooctyne (Tz-DBCO) by SPAAC, and subsequent IEDDA with trans-cyclooctene (TCO) functionalized NP. In contrast to using only metabolic azide labeling and subsequent conjugation of DBCO-NP, our 2-step method yields a highly specific cell surface conjugation of LNP, with very low non-specific background binding.

摘要

将纳米颗粒 (NP) 与活细胞表面缀合,对于利用体外工程化 T 细胞的组织归巢特性将药物负载到 NP 中,靶向递送至肿瘤是很有意义的。细胞表面缀合需要共价或非共价反应。用配体修饰的 NP (LNP) 的非共价缀合具有挑战性,并且涉及到结合态和非结合态之间的动态平衡。NP 的共价缀合导致 NP 处于永久结合状态,但目前用于细胞表面缀合的途径存在反应动力学缓慢和糖萼中蛋白质的随机缀合的问题。为了解决对允许有效共价细胞表面缀合的替代生物正交策略的未满足需求,我们开发了一种两步点击缀合序列,其中细胞首先通过代谢标记叠氮化物,然后通过 SPAAC 与磺基-6-甲基-四嗪-二苄基环辛炔 (Tz-DBCO) 反应,随后与反式环辛烯 (TCO) 功能化 NP 进行 IEDDA。与仅使用代谢叠氮化物标记和随后的 DBCO-NP 缀合相比,我们的两步法可高度特异性地将 LNP 缀合到细胞表面,非特异性背景结合非常低。

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