PROTAC-DB 3.0: an updated database of PROTACs with extended pharmacokinetic parameters

Author:

Ge Jingxuan12ORCID,Li Shimeng1,Weng Gaoqi1ORCID,Wang Huating1,Fang Meijing3,Sun Huiyong4ORCID,Deng Yafeng2,Hsieh Chang- Yu1,Li Dan1,Hou Tingjun13ORCID

Affiliation:

1. College of Pharmaceutical Sciences, Zhejiang University , Hangzhou 310058  Zhejiang , China

2. CarbonSilicon AI Technology Company , Ltd., Hangzhou  310018 Zhejiang , China

3. Polytechnic Institute, Zhejiang University , Hangzhou 310058  Zhejiang , China

4. Department of Medicinal Chemistry, China Pharmaceutical University , Nanjing 210009  Jiangsu , China

Abstract

Abstract Proteolysis-targeting chimera (PROTAC) is an emerging therapeutic technology that leverages the ubiquitin-proteasome system to target protein degradation. Due to its event-driven mechanistic characteristics, PROTAC has the potential to regulate traditionally non-druggable targets. Recently, AI-aided drug design has accelerated the development of PROTAC drugs. However, the rational design of PROTACs remains a considerable challenge. Here, we present an updated online database, PROTAC-DB 3.0. In this third version, we have expanded the database to include 6111 PROTACs (87% increase compared to the 2.0 version). Additionally, the database now contains 569 warheads (small molecules targeting the protein), 2753 linkers, and 107 E3 ligands (small molecules recruiting E3 ligases). The number of target-PROTAC-E3 ternary complex structures has also increased to 959. Recognizing the importance of druggability in PROTAC design, we have incorporated pharmacokinetic data to PROTAC-DB 3.0. To enhance user experience, we have added features for sorting based on molecular similarity and literature publication date. PROTAC-DB 3.0 is accessible at http://cadd.zju.edu.cn/protacdb/.

Funder

National Key Research and Development Program of China

National Natural Science Foundation of China

Natural Science Foundation of Zhejiang Province

Publisher

Oxford University Press (OUP)

Reference27 articles.

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