脂肪量和肥胖相关基因介导的血红素加氧酶-1 m6A 修饰在脊髓损伤小鼠神经功能恢复中的作用机制。

Mechanism of Fat Mass and Obesity-Related Gene-Mediated Heme Oxygenase-1 m6A Modification in the Recovery of Neurological Function in Mice with Spinal Cord Injury.

机构信息

Department of Spine Surgery, The First Affiliated Hospital, Sun Yat-sen University (Guangdong Provincial Key Laboratory of Orthopaedics and Traumatology), Guangzhou, China.

出版信息

Orthop Surg. 2024 May;16(5):1175-1186. doi: 10.1111/os.14002. Epub 2024 Mar 21.

DOI:10.1111/os.14002

PMID:38514911

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11062882/

Abstract

OBJECTIVES

This study examined the mechanism of fat mass and obesity-related gene (FTO)-mediated heme oxygenase-1 (HO-1) m6A modification facilitating neurological recovery in spinal cord injury (SCI) mice. FTO/HO-1 was identified as a key regulator of SCI as well as a potential target for treatment of SCI.

METHODS

An SCI mouse was treated with pcDNA3.1-FTO/pcDNA3.1-NC/Dac51. An oxygen/glucose deprivation (OGD) cell model simulated SCI, with cells treated with pcDNA3.1-FTO/si-HO-1/Dac51. Motor function and neurobehavioral evaluation were assessed using the Basso, Beattie, and Bresnahan (BBB) scale and modified neurological severity score (mNSS). Spinal cord pathology and neuronal apoptosis were assessed. Further, FTO/HO-1 mRNA and protein levels, HO-1 mRNA stability, the interaction of YTHDF2 with HO-1 mRNA, neuronal viability/apoptosis, and HO-1 m6A modification were evaluated.

RESULTS

Spinal cord injury mice exhibited reduced BBB, elevated mNSS scores, disorganized spinal cord cells, scattered nuclei, and severe nucleus pyknosis. pcDNA3.1-FTO elevated FTO mRNA, protein expression, and BBB score; reduced the mNSS score of SCI mice; decreased neuronal apoptosis; improved the cell arrangement; and improved nucleus pyknosis in spinal cord tissues. OGD decreased FTO expression. FTO upregulation ameliorated OGD-induced neuronal apoptosis. pcDNA3.1-FTO reduced HO-1 mRNA and protein and HO-1 m6A modification, while increasing HO-1 mRNA stability and FTO in OGD-treated cells. FTO upregulated HO-1 by modulating m6A modification. HO-1 downregulation attenuated the effect of FTO. pcDNA3.1-FTO/Dac51 increased the HO-1 m6A level in mouse spinal cord tissue homogenate, reduced BBB, boosted mNSS scores of SCI mice, aggravated nucleus pyknosis, and increased neuronal apoptosis in spinal cord tissues, confirming that FTO mediated HO-1 m6A modification facilitated neurological recovery in SCI mice.

CONCLUSION

The fat mass and obesity-related gene modulates HO-1 mRNA stability by regulating m6A modification levels, thereby influencing HO-1 expression and promoting neurological recovery in SCI mice.

摘要

目的

本研究旨在探讨肥胖相关基因（FTO）介导的血红素加氧酶-1（HO-1）m6A 修饰促进脊髓损伤（SCI）小鼠神经功能恢复的机制。FTO/HO-1 被鉴定为 SCI 的关键调节因子，也是 SCI 治疗的潜在靶点。

方法

采用 pcDNA3.1-FTO/pcDNA3.1-NC/Dac51 处理 SCI 小鼠。采用氧葡萄糖剥夺（OGD）细胞模型模拟 SCI，用 pcDNA3.1-FTO/si-HO-1/Dac51 处理细胞。采用 Basso、Beattie 和 Bresnahan（BBB）评分和改良神经功能严重程度评分（mNSS）评估运动功能和神经行为。评估脊髓病理和神经元凋亡。进一步评估 FTO/HO-1mRNA 和蛋白水平、HO-1mRNA 稳定性、YTHDF2 与 HO-1mRNA 的相互作用、神经元活力/凋亡以及 HO-1m6A 修饰。

结果

脊髓损伤小鼠 BBB 降低，mNSS 评分升高，脊髓细胞排列紊乱，细胞核散在，细胞核固缩严重。pcDNA3.1-FTO 升高 FTO mRNA、蛋白表达和 BBB 评分；降低 SCI 小鼠 mNSS 评分；减少神经元凋亡；改善脊髓组织细胞排列；减轻脊髓组织细胞核固缩。OGD 降低 FTO 表达。FTO 上调改善 OGD 诱导的神经元凋亡。pcDNA3.1-FTO 降低 HO-1mRNA 和蛋白及 HO-1m6A 修饰，同时增加 OGD 处理细胞中 HO-1mRNA 稳定性和 FTO。FTO 通过调节 m6A 修饰上调 HO-1。HO-1 下调减弱 FTO 的作用。pcDNA3.1-FTO/Dac51 增加小鼠脊髓组织匀浆中 HO-1m6A 水平，降低 BBB，提高 SCI 小鼠 mNSS 评分，加重脊髓组织细胞核固缩，增加神经元凋亡，证实 FTO 通过调节 HO-1m6A 修饰促进 SCI 小鼠神经功能恢复。