Structure and Function of the PR-DUB Complex and Its Role in the Development of Haematological Tumours
10.13865/j.cnki.cjbmb.2024.03.1410
- VernacularTitle:多梳抑制性去泛素化酶复合物的结构与功能及其在血液肿瘤发生发展中的作用
- Author:
Wen-Wen ZHANG
1
;
Fu-Quan JIANG
;
Zhen-Hua CHEN
Author Information
1. 江西科技师范大学药学院,江西省药物分子设计与评价重点实验室,南昌 330013
- Keywords:
polycomb repressive deubiquitinase complex(PR-DUB);
deubiquitination modification;
gene mutation;
hematologic tumors
- From:
Chinese Journal of Biochemistry and Molecular Biology
2024;40(7):879-888
- CountryChina
- Language:Chinese
-
Abstract:
The polycomb repressive deubiquitinase complex(PR-DUB)is a member of the polycomb group protein involved in the epigenetic modification of chromosomes by regulating histone modifications.The polycomb repressive complex 1(PRC1)and PR-DUB complex protect active genes from aberrant si-lencing through a balance of ubiquitination and deubiquitination modifications of H2AK119Ub.The deu-biquitination function of the PR-DUB complex is associated with the promotion of gene activation and the establishment of transcriptionally permissive chromatin states,in addition to the activation of enhancers and the facilitation of DNA damage repair at double-strand breaks.Additional sex combs-like 1(ASXL1)serves as an epigenetic scaffold for the assembly of chromatin-modifying complexes and tran-scription factors involved in epigenetic regulation.BRCA1-associated protein 1(BAP1)acts as a deubiq-uitinating enzyme to remove ubiquitination modification of substrates.The PR-DUB complex consists of a core dimer and other cofactors.BAP 1 forms a core dimer with ASXL1,and other subunits interact to reg-ulate the targeting and functioning of the PR-DUB complex.ASXL1 and BAP1 are the two subunits most relevant to the deubiquitination function of the PR-DUB complex,and the DEUBAD domain of ASXL1 activates BAP1 to exert its deubiquitination function to hydrolyze H2AK119Ub1.Understanding the struc-ture and interaction mechanism of ASXL1 and BAP1 is essential to study the mechanism of deubiquitina-tion specific to the PR-DUB complex.In humans,mutations in the components of the PR-DUB complex frequently cause a variety of hematologic neoplasms.Mutations in the ASSXL1 gene often result in prema-ture termination of protein translation,mostly due to the absence of the C-terminal PHD domain.The in-teraction of mutated ASXL1 or BAP1,epigenetic factors,and targets or signaling pathways such as Akt/mTOR in PR-DUB is now considered as a possible mechanism to promote the development of hematologi-cal tumors.This is crucial for the research and development of new specific targeted therapeutic agents a-gainst potential therapeutic targets.In this paper,focusing on ASXL1 and BAP1,we will introduce the structure and function of the PR-DUB complex,and its mechanism in the occurrence of hematological tumor diseases,and systematically summarize the potential targeted therapeutic drugs,with a view to pro-viding scientific references for the research of the PR-DUB complex in the prevention and treatment of he-matological diseases.
