Proteolysis targeting chimeras (PROTACs) are emerging therapeutics for hematologic malignancies

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作者
Yonghan He
Sajid Khan
Zhiguang Huo
Dongwen Lv
Xuan Zhang
Xingui Liu
Yaxia Yuan
Robert Hromas
Mingjiang Xu
Guangrong Zheng
Daohong Zhou
机构
[1] University of Florida,Department of Pharmacodynamics, College of Pharmacy
[2] University of Florida,Department of Biostatistics, College of Public Health & Health Professions and College of Medicine
[3] University of Florida,Department of Medicinal Chemistry, College of Pharmacy
[4] The University of Texas Health Science Center at San Antonio,Department of Medicine
[5] Department of Molecular Medicine,undefined
[6] College of Medicine,undefined
关键词
PROTAC; Cell-specific E3 ligases; Small molecule inhibitor; Hematologic malignancy;
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摘要
Proteolysis targeting chimeras (PROTACs) are heterobifunctional small molecules that utilize the ubiquitin proteasome system (UPS) to degrade proteins of interest (POI). PROTACs are potentially superior to conventional small molecule inhibitors (SMIs) because of their unique mechanism of action (MOA, i.e., degrading POI in a sub-stoichiometric manner), ability to target “undruggable” and mutant proteins, and improved target selectivity. Therefore, PROTACs have become an emerging technology for the development of novel targeted anticancer therapeutics. In fact, some of these reported PROTACs exhibit unprecedented efficacy and specificity in degrading various oncogenic proteins and have advanced to various stages of preclinical and clinical development for the treatment of cancer and hematologic malignancy. In this review, we systematically summarize the known PROTACs that have the potential to be used to treat various hematologic malignancies and discuss strategies to improve the safety of PROTACs for clinical application. Particularly, we propose to use the latest human pan-tissue single-cell RNA sequencing data to identify hematopoietic cell type-specific/selective E3 ligases to generate tumor-specific/selective PROTACs. These PROTACs have the potential to become safer therapeutics for hematologic malignancies because they can overcome some of the on-target toxicities of SMIs and PROTACs.
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