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用于组织蛋白酶B介导的无痕迹释放有效载荷的寡核苷酸-小分子缀合物的模块化自动化合成。

Modular and automated synthesis of oligonucleotide-small molecule conjugates for cathepsin B mediated traceless release of payloads.

作者信息

Jin Cheng, Li Siqi, Vallis Katherine A, El-Sagheer Afaf H, Brown Tom

机构信息

Department of Chemistry, Chemistry Research Laboratory, University of Oxford 12 Mansfield Road Oxford OX1 3TA UK

Hangzhou Institute of Medicine (HIM), Chinese Academy of Sciences, Zhejiang Cancer Hospital Hangzhou Zhejiang 310022 China

出版信息

RSC Chem Biol. 2024 May 29;5(8):738-744. doi: 10.1039/d4cb00112e. eCollection 2024 Jul 31.

Abstract

The reversible attachment of small molecules to oligonucleotides provides versatile tools for the development of improved oligonucleotide therapeutics. However, cleavable linkers in the oligonucleotide field are scarce, particularly with respect to the requirement for traceless release of the payload . Herein, we describe a cathepsin B-cleavable dipeptide phosphoramidite, Val-Ala(NB) for the automated synthesis of oligonucleotide-small molecule conjugates. Val-Ala(NB) was protected by a photolabile 2-nitrobenzyl group to improve the stability of the peptide linker during DNA synthesis. Intracellular cathepsin B digests the dipeptide efficiently, releasing the payload-phosphate which is converted to the free payload by endogenous phosphatase enzymes. With the advantages of modular synthesis and stimuli-responsive drug release, we believe Val-Ala(NB) will be a potentially valuable cleavable linker for use in oligonucleotide-drug conjugates.

摘要

小分子与寡核苷酸的可逆连接为开发改良的寡核苷酸疗法提供了多功能工具。然而,寡核苷酸领域中可裂解的连接子很少,特别是在对有效载荷无痕释放的要求方面。在此,我们描述了一种用于自动合成寡核苷酸 - 小分子缀合物的组织蛋白酶B可裂解的二肽亚磷酰胺,即Val - Ala(NB)。Val - Ala(NB)由光不稳定的2 - 硝基苄基保护,以提高肽连接子在DNA合成过程中的稳定性。细胞内的组织蛋白酶B可有效消化二肽,释放出有效载荷 - 磷酸酯,其通过内源性磷酸酶转化为游离的有效载荷。凭借模块化合成和刺激响应性药物释放的优势,我们相信Val - Ala(NB)将成为用于寡核苷酸 - 药物缀合物的潜在有价值的可裂解连接子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b99e/11289880/bb839ddef6f5/d4cb00112e-f1.jpg

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