刮痧疗法通过调节GLUT4/糖酵解和AMPK/mTOR/4EBP1通路促进腰椎多裂肌损伤大鼠肌肉再生。

IF 2.5 3区 医学 Q2 CLINICAL NEUROLOGY
Pain Research & Management Pub Date : 2023-06-22 eCollection Date: 2023-01-01 DOI:10.1155/2023/8870256
Bin Zou, Juan Du, Qiwen Xuan, Yajing Wang, Zixiao Wang, Wen Zhang, Lianghua Wang, Wei Gu
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引用次数: 0

摘要

背景:非特异性腰痛(NLBP)发病率高,医疗资源消耗大,已成为一种沉重的社会负担。诱发NLBP的因素很多,其中多裂肌的损伤和萎缩与NLBP关系最为密切。与其他方式或药物相比,刮痧疗法可以对NLBP产生显著的治疗效果,不良反应更少,医疗资金投入更少。然而,刮痧疗法治疗NLBP的机制尚不明确。在这里,我们想研究刮痧疗法对促进MF再生的影响及其潜在机制。方法:共54只雄性大鼠(SD,6-7 周龄)随机分为K、M6h、M1d、M2d、M3d、G6h、G1d、G2d和G3d 9组,每组6只。他们被注射了布比卡因(BPVC)以故意诱导MF损伤。然后,我们对随机选择的大鼠进行刮痧治疗,并比较不同时间点的治疗效果。收集体外数据,包括皮肤温度和触觉异常性疼痛阈值,并分析组织学切片。应用信使核糖核酸测序来区分因刮削治疗而改变的基因或信号通路,并通过逆转录聚合酶链式反应和蛋白质印迹分析进一步验证了结果。结果:刮痧法引起的大鼠皮肤上下的短暂性瘀点和瘀斑在3年左右逐渐消退 d.MF的横截面积(CSA)明显较小30 h、 2 d、 和4 建模后第d天(与空白组相比,分别为P=0.007、P=0.001和P=0.015),刮除组1中明显更大 d(与模型1d组相比P=0.002)。刮削后皮肤温度立即显著升高(P<0.001),后肢疼痛阈值在刮削后第2天升高(分别为P=0.046和P=0.028)。391个差异表达基因和8个信号通路被鉴定6 h刮除后;仅筛选出3个差异表达基因和3个信号通路 d。刮除治疗后,GLUT4、HK2、PFKM、PKM、LDHA(属于GLUT4/糖酵解途径)、p-mTOR、p-4EBP1(属于AMPK/mTOR/4EBP1途径)和BDH1的mRNA或蛋白质数量增加,p-AMPKα减少。结论:刮痧疗法通过调节GLUT4/糖酵解和AMPK/mTOR/4EBP1信号通路促进肌肉再生,对多裂肌损伤大鼠具有治疗作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Scraping Therapy Improved Muscle Regeneration through Regulating GLUT4/Glycolytic and AMPK/mTOR/4EBP1 Pathways in Rats with Lumbar Multifidus Injury.

Scraping Therapy Improved Muscle Regeneration through Regulating GLUT4/Glycolytic and AMPK/mTOR/4EBP1 Pathways in Rats with Lumbar Multifidus Injury.

Scraping Therapy Improved Muscle Regeneration through Regulating GLUT4/Glycolytic and AMPK/mTOR/4EBP1 Pathways in Rats with Lumbar Multifidus Injury.

Scraping Therapy Improved Muscle Regeneration through Regulating GLUT4/Glycolytic and AMPK/mTOR/4EBP1 Pathways in Rats with Lumbar Multifidus Injury.

Background: High morbidity of nonspecific low back pain (NLBP) and large consumption of medical resources caused by it have become a heavy social burden. There are many factors inducing NLBP, among which the damage and atrophy of multifidus (MF) are most closely related to NLBP. Scraping therapy can have significant treatment effects on NLBP with fewer adverse reactions and less medical fund input than other modalities or medications. However, the mechanism of scraping therapy treating NLBP remains unclarified. Here, we wanted to investigate the effects of scraping therapy on promoting MF regeneration and the underlying mechanisms.

Methods: A total of 54 male rats (SD, 6-7 weeks old) were randomly divided into nine groups, namely, K, M6h, M1d, M2d, M3d, G6h, G1d, G2d, and G3d, with six rats in each group. They were injected with bupivacaine (BPVC) to intentionally induce MF injury. We then performed scraping therapy on the rats that had been randomly chosen and compared treatment effects at different time points. In vitro data including skin temperature and tactile allodynia threshold were collected and histological sections were analyzed. mRNA sequencing was applied to distinguish the genes or signaling pathways that had been altered due to scraping therapy, and the results were further verified through reverse transcription polymerase chain reaction and Western blot analysis.

Results: Transitory petechiae and ecchymosis both on and beneath the rats' skin raised by scraping therapy gradually faded in about 3 d. Cross-sectional area (CSA) of MF was significantly smaller 30 h, 2 d, and 4 d after modeling (P=0.007, P=0.001, and P=0.015, respectively, vs. the blank group) and was significantly larger in the scraping group 1 d after treatment (P=0.002 vs. the model 1d group). Skin temperature significantly increased immediately after scraping (P < 0.001) and hindlimb pain threshold increased on the 2nd day after scraping (P=0.046 and P=0.028, respectively). 391 differentially expressed genes and 8 signaling pathways were characterized 6 h after scraping; only 3 differentially expressed genes and 3 signaling pathways were screened out 2 d after treatment. The amounts of mRNAs or proteins for GLUT4, HK2, PFKM, PKM, LDHA (which belong to the GLUT4/glycolytic pathway), p-mTOR, p-4EBP1 (which belong to the AMPK/mTOR/4EBP1 pathway), and BDH1 were enhanced, and p-AMPKα was decreased after scraping therapy.

Conclusions: Scraping therapy has therapeutic effects on rats with multifidus injury by promoting muscle regeneration via regulating GLUT4/glycolytic and AMPK/mTOR/4EBP1 signaling pathways.

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来源期刊
Pain Research & Management
Pain Research & Management CLINICAL NEUROLOGY-
CiteScore
5.30
自引率
0.00%
发文量
109
审稿时长
>12 weeks
期刊介绍: Pain Research and Management is a peer-reviewed, Open Access journal that publishes original research articles, review articles, and clinical studies in all areas of pain management. The most recent Impact Factor for Pain Research and Management is 1.685 according to the 2015 Journal Citation Reports released by Thomson Reuters in 2016.
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