Journal article

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

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 in vivo. 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.

Publication status:: Published

Peer review status:: Peer reviewed

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APA Style

Jin, C., Li, S., Vallis, K. A., El-Sagheer, A. H., & Brown, T. (2024). Modular and automated synthesis of oligonucleotide-small molecule conjugates for cathepsin B mediated traceless release of payloads † ‡. RSC Chemical Biology.

MLA Style

Jin, C., et al. “Modular and Automated Synthesis of Oligonucleotide-Small Molecule Conjugates for Cathepsin B Mediated Traceless Release of Payloads † ‡.” RSC Chemical Biology, Royal Society of Chemistry, 2024.

Chicago Style

Jin, C, S Li, KA Vallis, AH El-Sagheer, and T Brown. 2024. “Modular and Automated Synthesis of Oligonucleotide-Small Molecule Conjugates for Cathepsin B Mediated Traceless Release of Payloads † ‡.” RSC Chemical Biology.
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Files:: Jin_et_al_2024_Modular_and_automated.pdf

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Publisher copy:: 10.1039/d4cb00112e

Authors

+ Jin, C More by this author

Institution:: University of Oxford
Division:: HUMS
Department:: Classics Faculty
Sub department:: Chemistry Research Laboratory
Role:: Author

+ Li, S More by this author

Institution:: University of Oxford
Role:: Author
ORCID:: 0000-0002-6166-8421

+ Vallis, KA More by this author

Institution:: University of Oxford
Role:: Author
ORCID:: 0000-0003-4672-5683

+ El-Sagheer, AH More by this author

Institution:: University of Oxford
Division:: HUMS
Department:: Classics Faculty
Sub department:: Chemistry Research Laboratory
Role:: Author

+ Brown, T More by this author

Institution:: University of Oxford
Division:: HUMS
Department:: Classics Faculty
Sub department:: Chemistry Research Laboratory
Role:: Author
ORCID:: 0000-0002-6538-3036

Publisher:: Royal Society of Chemistry
Journal:: RSC Chemical Biology More from this journal
Publication date:: 2024-05-29
Acceptance date:: 2024-05-28
DOI:: 10.1039/d4cb00112e
EISSN:: 2633-0679
ISSN:: 2633-0679

Language:: English
Pubs id:: 2009042
Local pid:: pubs:2009042
Source identifiers:: 2049163
Deposit date:: 2024-06-18

Terms of use

Copyright date:: 2024

Licence:: CC Attribution (CC BY) 3.0

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