张冰玉; 李一帆; 李文君; 徐洁; 江潇; 井亮; 汪凯; 章娟娟

doi:10.3760/cma.j.cn371468-20221116-00688

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• 基础研究 •

前扣带回调控慢性非特异性腰痛模型大鼠疼痛及焦虑样行为的机制研究

中华行为医学与脑科学杂志, 2023,32(6) : 513-520. DOI: 10.3760/cma.j.cn371468-20221116-00688

摘要

目的

探讨前扣带回(anterior cingulate cortex，ACC)调控神经生长因子(nerve growth factor，NGF)诱导的慢性非特异性腰痛大鼠痛行为与焦虑样行为的潜在机制。

方法

成年雄性8周龄SPF级SD大鼠96只，按照随机数字表法分为4组(每组24只)：对照组、模型组、对照+D-AP5组(D-AP5为N-甲基-D-天冬氨酸受体拮抗剂)和模型+D-AP5组。采用第5腰椎左侧多裂肌注射NGF建立腰痛大鼠模型(注射2次，间隔5 d)。造模5 d后，对照+D-AP5组和模型+D-AP5组大鼠右侧前扣带回注射D-AP5(2 μg，0.3 μL，1次/d，连续3 d)，模型组和对照组则注射等体积0.9%氯化钠溶液。采用机械刺激和冷热板实验评估大鼠疼痛阈值，旷场实验评估大鼠焦虑样行为，免疫荧光法检测脊髓胶质纤维酸性蛋白(glial fibrillary acidic protein，GFAP)阳性细胞和c-Fos(一种即早基因)阳性细胞密度，Western blot实验检测脊髓GFAP、c-Fos蛋白、磷酸化c-Jun氨基末端激酶(phosphorylated c-Jun N-terminal kinases，p-JNK)、单核细胞趋化蛋白-1 (monocyte chemoattractant protein-1，MCP-1)和趋化因子(C-X-C基序)配体1[chemokine (C-X-C motif) ligand 1，CXCL-1]的表达。采用SPSS 23.0软件进行统计分析，正态分布的数据组间比较采用单因素方差分析，进一步两两比较采用Tukey检验；非正态分布的数据组间比较采用Krusal-Wallis H检验，两两比较采用Mann-Whitney U检验并对P值进行Bonferroni校正。

结果

4组大鼠腰部压力疼痛阈值(pressure pain threshold，PPT)、机械缩足阈值(paw withdrawal threshold，PWT)均差异有统计学意义(F＝53.498，41.939，均P<0.001)。造模后7 d，模型+D-AP5组PPT[(418.5±46.9)g]、足底PWT[(55.6±7.1)g]均高于模型组[(290.0±32.0)g，(30.5±7.5)g](均P<0.001)。各组旷场实验中央区活动距离百分比(H＝11.922，P<0.01)、中央区活动时间百分比(H＝21.614，P<0.001)均差异有统计学意义。模型+D-AP5组中央区活动时间百分比高于模型组[5.6(4.3，7.9)%，3.1(2.1，3.8)%](P<0.01)。各组左侧脊髓背角浅层GFAP、c-Fos阳性细胞密度均差异有统计学意义(H＝49.085，F＝18.120，均P<0.001)。模型+D-AP5组左侧背角浅层GFAP [34.3(21.1，47.5)个/mm²]、c-Fos阳性细胞密度[(52.7±39.4)个/mm²]低于模型组[76.5(68.6，94.9)个/mm²，(112.4±63.7)个/mm²](均P<0.001)。各组腰2节段GFAP、c-Fos、p-JNK、MCP-1、CXCL-1蛋白表达均差异有统计学意义(F＝49.413，38.437，41.867，36.735，130.951，均P<0.001)。模型+D-AP5组腰2节段GFAP(1.7±0.5)、c-Fos(1.1±0.1)、p-JNK(1.7±0.3)、MCP-1(1.0±0.4)、CXCL-1(0.8±0.1)蛋白表达均低于模型组[(4.3±0.7)，(2.6±0.5)，(2.8±0.4)，(2.9±0.4)，(3.5±0.4)](均P<0.01)。

结论

ACC可调控慢性非特异性腰痛大鼠机械性痛觉过敏及焦虑样行为，这可能与脊髓星形胶质细胞、p-JNK通路、MCP-1和CXCL1的参与有关。

引用本文: 张冰玉, 李一帆, 李文君, 等. 前扣带回调控慢性非特异性腰痛模型大鼠疼痛及焦虑样行为的机制研究 [J] . 中华行为医学与脑科学杂志, 2023, 32(6) : 513-520. DOI: 10.3760/cma.j.cn371468-20221116-00688.

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慢性腰痛非常普遍，给社会和家庭带来沉重的负担^[1]。椎体稳定性下降、椎间盘变性、肿瘤、感染等原因仅能解释部分慢性腰痛，而大部分腰痛无法归因于某种特异的病理性因素，这部分腰痛被称为慢性非特异性腰痛^[2,3]。神经生长因子(nerve growth factor，NGF)与肌肉疼痛密切相关，临床研究发现NGF抗体可缓解部分类型慢性腰痛^[4]，然而将肌肉作为慢性非特异性腰痛来源的基础研究较少，2013年Hoheisel等^[5]构建了NGF诱导的腰痛模型，该模型通过向大鼠第5腰椎多裂肌注射两次NGF，诱导长达14 d的脊髓背角神经元敏化和腰部痛觉过敏，而星形胶质细胞的活化维持了这一过程^[2]。功能磁共振研究发现，慢性腰痛患者前扣带回(anterior cingulate cortex，ACC)的低频振幅显著增加^[6]。作为情绪调节的高级中枢^[7]，ACC同时与下丘脑、杏仁核、中脑导水管周围灰质、延脑头端腹内侧核群、孤束核和背侧网状核等组成痛觉下行易化系统^[8,9]，该系统的正反馈环路持续诱发和维持慢性疼痛^[10,11]，因此ACC的激活与慢性腰痛关系密切。

贡献者信息

张冰玉

安徽医科大学第一附属医院神经内科，合肥　230022

李一帆

安徽医科大学第一附属医院神经内科，合肥　230022

李文君

安徽医科大学精神卫生与心理科学学院，合肥　230032

徐洁

安徽医科大学第一附属医院神经内科，合肥　230022

江潇

安徽医科大学精神卫生与心理科学学院，合肥　230032

井亮

安徽医科大学精神卫生与心理科学学院，合肥　230032

汪凯

安徽医科大学第一附属医院神经内科，合肥　230022

章娟娟

安徽医科大学第一附属医院神经内科，合肥　230022

通信作者

章娟娟

安徽医科大学第一附属医院神经内科，合肥　230022

Email：zhangjuanjuan0207@126.com

关键词

前扣带回; 慢性非特异性腰痛; 神经生长因子; 焦虑; 星形胶质细胞; 痛觉过敏; 大鼠;

基金项目

国家自然科学基金（81901135）

安徽省教育厅科学研究项目（KJ2019A0243）

作者声明

作者贡献声明

张冰玉：实验操作、采集数据、数据统计分析、论文撰写；李一帆：实验操作、采集数据、数据统计分析；李文君、徐洁：实验操作、采集数据；江潇、井亮、汪凯：实验设计、论文修改、研究指导；章娟娟：实验设计、研究指导、论文修改、经费支持

利益冲突

所有作者均声明不存在利益冲突

历史

出版日期：2023-06-20

收稿日期：2022-11-16

本文编辑

张敬美

Basic Research

Mechanism of anterior cingulate cortex in modulating pain and anxiety-like behavior in chronic non-specific low back pain model rats

Zhang Bingyu, Li Yifan, Li Wenjun, Xu Jie, Jiang Xiao, Jing Liang, Wang Kai, Zhang Juanjuan

Published 2023-06-20

Cite as Chin J Behav Med & Brain Sci, 2023, 32(6): 513-520. DOI: 10.3760/cma.j.cn371468-20221116-00688

Abstract

Objective

To explore the potential mechanisms of anterior cingulate cortex (ACC) in modulating pain behavior and anxiety-like behavior of rats with chronic non-specific low back pain induced by nerve growth factor (NGF).

Methods

Ninety-six male SPF grade SD rats aged 8 weeks were randomly divided into four groups according the random number table method: control group, model group, control+ D-2-amino-5-phosphonopentanoate (D-AP5) group (control+ D-AP5 group) and model+ D-AP5 group, with 24 rats in each group.Low back pain model of rat was established by injection of NGF into multifidus muscle (left side) of the low backs of rats(two times with a five-day interval). Five days after modeling, rats in model+ D-AP5 group and control+ D-AP5 group were injected with the N-methyl-D-aspartate (NMDA) receptor antagonist D-AP5(2 μg, 0.3 μL) at the right side of the ACC once a day for consecutive 3 days, and rats in control group and model group were injected with the same amount of 0.9% sodium chloride solution. Seven days after modeling, the pain threshold of rats was evaluated by mechanical stimulation test and hot and cold plate test.The anxiety-like behavior was tested by open field test.The density of glial fibrillary acidic protein (GFAP) positive cells and c-Fos(a kind of immediate early gene) positive cells of the spinal cord were observed by immunofluorescence. The expression of GFAP, c-Fos, phosphorylated-c-Jun N-terminal kinases (p-JNK), monocyte chemoattractant protein-1 (MCP-1), and chemokine (C-X-C motif) ligand 1 (CXCL-1) proteins in the L2 segment of the spinal cord were detected by Western blot. SPSS 23.0 software was used for statistical analysis. One-way ANOVA was used to analyze normal distribution measurement data for comparison among multiple groups, and Tukey test was used for further pairwise comparisons. The Kruakal-Wallis H test was used for non-normal distribution measurement data, and Mann-Whitney U test was used for further pairwise comparisons with Bonferroni-corrected P-values.

Results

In the experiments measuring pressure pain threshold (PPT) and paw withdrawal threshold (PWT), there were statistically significant differences in the PPT and PWT of rats among the four groups (F=53.498, 41.939, both P<0.001). Seven days after modeling, PPT ((418.5±46.9) g) and PWT ( (55.6±7.1) g) in the ipsilateral side of the rats in model+ D-AP5 group were higher than those in model group ((290.0±32.0) g, (30.5±7.5) g) (both P<0.001). In the open field test, there were statistically significant differences in percentage of the inner zone distance (H=11.922, P<0.01) and the percentage of inner zone time (H=21.614, P<0.001) of rats among the four groups. The percentage of inner zone time in model+ D-AP5 group was higher than that in model group (5.6(4.3, 7.9) %, 3.1(2.1, 3.8) %) (P<0.01). The results of immunofluorescence showed that there were statistically significant differences in the density of GFAP positive cells and c-Fos positive cells at the ipsilateral side of the superficial laminae of rats among the four groups (H=49.085, F=18.120, both P<0.001). The density of GFAP positive cells (34.3(21.1, 47.5) cells/mm²) and c-Fos positive cells ((52.7±39.4) cells/mm²) at the ipsilateral side of the superficial laminae in model+ D-AP5 group were less than those in model group (76.5(68.6, 94.9) cells/mm², (112.4±63.7) cells/mm²) (both P<0.001). The Western blot results showed that there were statistically significant differences in the protein expression of GFAP, c-Fos, p-JNK, MCP-1 and CXCL-1 in the L2 segment of rats among the four groups (F=49.413, 38.437, 41.867, 36.735, 130.951, all P<0.001). The protein expression of GFAP (1.7±0.5), c-Fos (1.1±0.1), p-JNK (1.7±0.3), MCP-1 (1.0±0.4) and CXCL-1 (0.8±0.1) in the L2 segment in model+ D-AP5 group were lower than those in model group ((4.3±0.7), (2.6±0.5), (2.8±0.4), (2.9±0.4), (3.5±0.4)) (all P<0.01).

Conclusion

ACC modulates mechanical hyperalgesia and anxiety-like behavior in chronic non-specific low back pain rats, which might be associated with the involvement of spinal astrocytes, p-JNK signal pathway and chemokines such as MCP-1 and CXCL-1.

Key words:

Anterior cingulate cortex; Chronic non-specific low back pain; Nerve growth factor; Anxiety; Astrocyte; Hyperalgesia; Rat

Contributor Information

Zhang Bingyu