Intracellular Delivery of Antisense Oligonucleotides by Tri‐Branched Cyclic Disulfide Units

Author:

Lyu Fangjie1,Hakariya Hayase1ORCID,Hiraoka Haruka1ORCID,Li Zhenmin1ORCID,Matsubara Noriaki1,Soo Yonghao1,Hashiya Fumitaka2ORCID,Abe Naoko1ORCID,Shu Zhaoma1,Nakamoto Kosuke1,Kimura Yasuaki1ORCID,Abe Hiroshi123ORCID

Affiliation:

1. Department of Chemistry Graduate School of Science Nagoya University Nagoya, Aichi 464-8602 Japan

2. Research Center for Materials Science Nagoya University Nagoya, Aichi 464-8602 Japan

3. Institute for Glyco-core Research (iGCORE) Nagoya University Nagoya, Aichi 464-8601 Japan

Abstract

AbstractTherapeutic oligonucleotides, such as antisense DNA, show promise in treating previously untreatable diseases. However, their applications are still hindered by the poor membrane permeability of naked oligonucleotides. Therefore, it is necessary to develop efficient methods for intracellular oligonucleotide delivery. Previously, our group successfully developed disulfide‐based Membrane Permeable Oligonucleotides (MPON), which achieved enhanced cellular uptake and gene silencing effects through an endocytosis‐free uptake mechanism. Herein, we report a new molecular design for the next generation of MPON, called trimer MPON. The trimer MPON consists of a tri‐branched backbone, three α‐lipoic acid units, and a spacer linker between the oligonucleotides and tri‐branched cyclic disulfide unit. We describe the design, synthesis, and functional evaluation of the trimer MPON, offering new insights into the molecular design for efficient oligonucleotide delivery.

Funder

Japan Science and Technology Agency

Ministry of Education, Culture, Sports, Science and Technology

Nagoya University

Publisher

Wiley

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