Aptamer‐LYTACs for Targeted Degradation of Extracellular and Membrane Proteins

Author:

Wu Yuqi1,Lin Bingqian2,Lu Yinzhu1,Li Liang1,Deng Kunyue1,Zhang Suhui1,Zhang Huiming3,Yang Chaoyong13,Zhu Zhi1ORCID

Affiliation:

1. The MOE Key Laboratory of Spectrochemical Analysis & Instrumentation the Key Laboratory of Chemical Biology of Fujian Province State Key Laboratory of Physical Chemistry of Solid Surfaces Department of Chemical Biology College of Chemistry and Chemical Engineering Xiamen University Xiamen China

2. College of Chemistry and Molecular Sciences Wuhan University Wuhan China

3. Innovation Laboratory for Sciences and Technologies of Energy Materials of Fujian Province Xiamen China

Abstract

AbstractRecently, lysosome targeting chimeras (LYTACs) have emerged as a promising technology that expands the scope of targeted protein degradation to extracellular targets. However, the preparation of chimeras by conjugation of the antibody and trivalent N‐acetylgalactosamine (tri‐GalNAc) is a complex and time‐consuming process. The large uncertainty in number and position and the large molecular weights of the chimeras result in low internalization efficiency. To circumvent these problems, we developed the first aptamer‐based LYTAC (Apt‐LYTAC) to realize liver‐cell‐specific degradation of extracellular and membrane proteins by conjugating aptamers to tri‐GalNAc. Taking advantage of the facile synthesis and low molecular weight of the aptamer, the Apt‐LYTACs can efficiently and quickly degrade the extracellular protein PDGF and the membrane protein PTK7 through a lysosomal degradation pathway. We anticipate that the novel Apt‐LYTACs will expand the usage of aptamers and provide a new dimension for targeted protein degradation.

Funder

Key Technologies Research and Development Program

National Natural Science Foundation of China

Central University Basic Research Fund of China

National Fund for Fostering Talents of Basic Science

Publisher

Wiley

Subject

General Chemistry,Catalysis

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