USP24-dependent stabilization of Runx2 recruits a p300/NCOA3 complex to transactivate ADAMTS genes and promote degeneration of intervertebral disc in chronic inflammation mice
BackgroundIntervertebral disc degeneration (IDD) naturally occurs during the aging process. Its occurrence is closely related to chronic inflammation; however, the causal relationship between them is controversial. This study aimed to investigate if inflammation would promote IDD incidence and explore the underlying mechanism.MethodsA chronic inflammation mouse model was established by intraperitoneal injection of lipopolysaccharide (LPS). Enzyme-linked immunosorbent assay was performed to determine proinflammatory cytokines in serum. Histological staining was used to evaluate the degeneration of IVDs. Immunoblots and RT-qPCR analyses were performed to measure protein and mRNA expression levels. Immunoprecipitation, mass spectrometry, and co-immunoprecipitation assays were used to determine the assembly of protein complex.ResultsWe found that an inflammatory microenvironment activated p38 kinase, which phosphorylated the Runx2 transcription factor at the Ser28 site. The phosphorylated Runx2 (pRunx2) then recruited a deubiquitinase, ubiquitin-specific peptidase 24 (USP24), which stabilized pRunx2 and protected it from ubiquitin-dependent proteasomal degradation. The stabilized pRunx2 recruited histone acetyltransferase p300 and nuclear receptor coactivator 3 (NCOA3) to assemble a complex. This NCOA3-p300-pRunx2 complex then transactivated the expression of 13 ADAMTS (a disintegrin and metalloproteinase with thrombospondin motif) genes, thereby promoting the degradation of extracellular matrix (ECM) in intervertebral discs (IVDs) and causing IDD. Administration of either a p38 inhibitor (doramapimod), a NCOA3 inhibitor (bufalin), or a p300 inhibitor (EML425) significantly decreased the expression of the 13 ADAMTS genes and slowed the degeneration of IVDs.ConclusionIn summary, our results demonstrate that USP24 protects pRunx2 from proteasomal degradation under chronic inflammation conditions, enabling pRunx2 to transactivate ADAMTS genes and degrade ECM. Our findings provide direct evidence that chronic inflammation triggers IDD and offer a therapeutic strategy for retarding IDD in patients with chronic inflammation.
基金:
National Natural Science Foundation of China [82160428, 82260449]; Yunnan health~training project of high-level talents [H-2017065, H-2019012]; Major Science and Technology Project of Yunnan Provincial Department of Science and Technology and Yunnan Provincial Orthopedic and Sports Rehabilitation Clinical Medicine Research Center [202102AA310068]; Yunnan Provincial Clinical Medical Center for Bone and Joint Diseases [ZX2019-03-04]; 535 Talent Project of First Affiliated Hospital of Kunming Medical University [2022535D10]; Joint Project on Applied Basic Research Foundation of Yunnan Science and Technology Department-Kunming Medical University [202101AY070001-120]
第一作者机构:[1]Kunming Med Univ, Affiliated Hosp 1, Dept Orthoped, Kunming 650032, Yunnan, Peoples R China
通讯作者:
推荐引用方式(GB/T 7714):
Li Xingguo,Zhang Jun,Wang Bing,et al.USP24-dependent stabilization of Runx2 recruits a p300/NCOA3 complex to transactivate ADAMTS genes and promote degeneration of intervertebral disc in chronic inflammation mice[J].BIOLOGY DIRECT.2023,18(1):doi:10.1186/s13062-023-00395-5.
APA:
Li, Xingguo,Zhang, Jun,Wang, Bing,Chen, Chao,Zhang, Enyu...&Zhang, Fan.(2023).USP24-dependent stabilization of Runx2 recruits a p300/NCOA3 complex to transactivate ADAMTS genes and promote degeneration of intervertebral disc in chronic inflammation mice.BIOLOGY DIRECT,18,(1)
MLA:
Li, Xingguo,et al."USP24-dependent stabilization of Runx2 recruits a p300/NCOA3 complex to transactivate ADAMTS genes and promote degeneration of intervertebral disc in chronic inflammation mice".BIOLOGY DIRECT 18..1(2023)
