Beyond canonical PROTAC: biological targeted protein degradation (bioTPD)

被引:0
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作者
Huifang Wang
Runhua Zhou
Fushan Xu
Kongjun Yang
Liuhai Zheng
Pan Zhao
Guangwei Shi
Lingyun Dai
Chengchao Xu
Le Yu
Zhijie Li
Jianhong Wang
Jigang Wang
机构
[1] Shenzhen People’s Hospital,Shenzhen Institute of Respiratory Disease, Shenzhen Clinical Research Centre for Respirology, The Second Clinical Medical College, The First Affiliated Hospital
[2] Jinan University,School of Pharmaceutical Science
[3] Southern University of Science and Technology,The Second Clinical Medical College, The First Affiliated Hospital
[4] Southern Medical University,State Key Laboratory for Quality Ensurance and Sustainable Use of Dao
[5] Shenzhen People’s Hospital,di Herbs
[6] Jinan University,Shenzhen Mental Health Center
[7] Southern University of Science and Technology,undefined
[8] Artemisinin Research Center,undefined
[9] and Institute of Chinese Materia Medica,undefined
[10] China Academy of Chinese Medical Sciences,undefined
[11] Shenzhen Kangning Hospital,undefined
来源
关键词
Biological targeted protein degradation (bioTPD); Peptide; Antibody; Fusion protein; Nucleic acid;
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摘要
Targeted protein degradation (TPD) is an emerging therapeutic strategy with the potential to modulate disease-associated proteins that have previously been considered undruggable, by employing the host destruction machinery. The exploration and discovery of cellular degradation pathways, including but not limited to proteasomes and lysosome pathways as well as their degraders, is an area of active research. Since the concept of proteolysis-targeting chimeras (PROTACs) was introduced in 2001, the paradigm of TPD has been greatly expanded and moved from academia to industry for clinical translation, with small-molecule TPD being particularly represented. As an indispensable part of TPD, biological TPD (bioTPD) technologies including peptide-, fusion protein-, antibody-, nucleic acid-based bioTPD and others have also emerged and undergone significant advancement in recent years, demonstrating unique and promising activities beyond those of conventional small-molecule TPD. In this review, we provide an overview of recent advances in bioTPD technologies, summarize their compositional features and potential applications, and briefly discuss their drawbacks. Moreover, we present some strategies to improve the delivery efficacy of bioTPD, addressing their challenges in further clinical development.
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