Affiliation:
1. Department of Orthopedics Taizhou School of Clinical Medicine Taizhou People's Hospital of Nanjing Medical University, Nanjing Medical University Taizhou China
2. Department of Spine Surgery Nantong First People's Hospital The Second Affiliated Hospital of Nantong University Nantong China
3. Postgraduate School Dalian Medical University Dalian China
4. Department of Trauma and Reconstructive Surgery RWTH Aachen University Hospital Aachen Germany
Abstract
AbstractBackgroundSpinal cord injury (SCI)‐induced neuroinflammation and oxidative stress (OS) are crucial events causing neurological dysfunction. Aconitate decarboxylase 1 (ACOD1) and its metabolite itaconate (Ita) inhibit inflammation and OS by promoting alkylation of Keap1 to induce Nrf2 expression; however, it is unclear whether there is another pathway regulating their effects in inflammation‐activated microglia after SCI.MethodsAdult male C57BL/6 ACOD1−/− mice and their wild‐type (WT) littermates were subjected to a moderate thoracic spinal cord contusion. The degree of neuroinflammation and OS in the injured spinal cord were assessed using qPCR, western blot, flow cytometry, immunofluorescence, and trans‐well assay. We then employed immunoprecipitation‐western blot, chromatin immunoprecipitation (ChIP)‐PCR, dual‐luciferase assay, and immunofluorescence‐confocal imaging to examine the molecular mechanisms of ACOD1. Finally, the locomotor function was evaluated with the Basso Mouse Scale and footprint assay.ResultsBoth in vitro and in vivo, microglia with transcriptional blockage of ACOD1 exhibited more severe levels of neuroinflammation and OS, in which the expression of p62/Keap1/Nrf2 was down‐regulated. Furthermore, silencing ACOD1 exacerbated neurological dysfunction in SCI mice. Administration of exogenous Ita or 4‐octyl itaconate reduced p62 phosphorylation. Besides, ACOD1 was capable of interacting with phosphorylated p62 to enhance Nrf2 activation, which in turn further promoted transcription of ACOD1.ConclusionsHere, we identified an unreported ACOD1‐p62‐Nrf2‐ACOD1 feedback loop exerting anti‐inflammatory and anti‐OS in inflammatory microglia, and demonstrated the neuroprotective role of ACOD1 after SCI, which was different from that of endogenous and exogenous Ita. The present study extends the functions of ACOD1 and uncovers marked property differences between endogenous and exogenous Ita.Key points
ACOD1 attenuated neuroinflammation and oxidative stress after spinal cord injury.
ACOD1, not itaconate, interacted with p‐p62 to facilitate Nrf2 expression and nuclear translocation.
Nrf2 was capable of promoting ACOD1 transcription in microglia.
Funder
Basic Research Program of Jiangsu Province
China Postdoctoral Science Foundation