TRAP1 drives smooth muscle cell senescence and promotes atherosclerosis via HDAC3-primed histone H4 lysine 12 lactylation

Xuesong Li; Minghong Chen; Xiang Chen; Xian He; Xinyu Li; Huiyuan Wei; Yongkang Tan; Jiao Min; Tayyiba Azam; Mengdie Xue; Yunjia Zhang; Mengdie Dong; Quanwen Yin; Longbin Zheng; Hong Jiang; Da Huo; Xin Wang; Shaoliang Chen; Yong Ji; Hongshan Chen

doi:10.1093/eurheartj/ehae379

TRAP1 drives smooth muscle cell senescence and promotes atherosclerosis via HDAC3-primed histone H4 lysine 12 lactylation

Xuesong Li(Nanjing Medical University), Minghong Chen(Nanjing Medical University), Xiang Chen(Nanjing Medical University), Xian He(Nanjing Medical University), Xinyu Li(Nanjing Medical University), Huiyuan Wei(Nanjing Medical University), Yongkang Tan(Nanjing Medical University), Jiao Min(Nanjing Medical University), Tayyiba Azam(University of Manchester), Mengdie Xue(Nanjing Medical University), Yunjia Zhang(Nanjing Medical University), Mengdie Dong(Nanjing Medical University), Quanwen Yin(Nanjing Medical University), Longbin Zheng(Nanjing Medical University), Hong Jiang(Nanjing Medical University), Da Huo(Nanjing Medical University), Xin Wang(University of Manchester), Shaoliang Chen(Nanjing Medical University), Yong Ji(Ministry of Education of the People's Republic of China), Hongshan Chen(Jiangsu Province Hospital)

European Heart Journal

August 1, 2024

10.1093/eurheartj/ehae379

Cited by 140Open Access

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Abstract

BACKGROUND AND AIMS: Vascular smooth muscle cell (VSMC) senescence is crucial for the development of atherosclerosis, characterized by metabolic abnormalities. Tumour necrosis factor receptor-associated protein 1 (TRAP1), a metabolic regulator associated with ageing, might be implicated in atherosclerosis. As the role of TRAP1 in atherosclerosis remains elusive, this study aimed to examine the function of TRAP1 in VSMC senescence and atherosclerosis. METHODS: TRAP1 expression was measured in the aortic tissues of patients and mice with atherosclerosis using western blot and RT-qPCR. Senescent VSMC models were established by oncogenic Ras, and cellular senescence was evaluated by measuring senescence-associated β-galactosidase expression and other senescence markers. Chromatin immunoprecipitation (ChIP) analysis was performed to explore the potential role of TRAP1 in atherosclerosis. RESULTS: VSMC-specific TRAP1 deficiency mitigated VSMC senescence and atherosclerosis via metabolic reprogramming. Mechanistically, TRAP1 significantly increased aerobic glycolysis, leading to elevated lactate production. Accumulated lactate promoted histone H4 lysine 12 lactylation (H4K12la) by down-regulating the unique histone lysine delactylase HDAC3. H4K12la was enriched in the senescence-associated secretory phenotype (SASP) promoter, activating SASP transcription and exacerbating VSMC senescence. In VSMC-specific Trap1 knockout ApoeKO mice (ApoeKOTrap1SMCKO), the plaque area, senescence markers, H4K12la, and SASP were reduced. Additionally, pharmacological inhibition and proteolysis-targeting chimera (PROTAC)-mediated TRAP1 degradation effectively attenuated atherosclerosis in vivo. CONCLUSIONS: This study reveals a novel mechanism by which mitonuclear communication orchestrates gene expression in VSMC senescence and atherosclerosis. TRAP1-mediated metabolic reprogramming increases lactate-dependent H4K12la via HDAC3, promoting SASP expression and offering a new therapeutic direction for VSMC senescence and atherosclerosis.

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