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The Roles of Chemokine CXCL13 in the Development of Bone Cancer Pain and the Regulation of Morphine Analgesia in Rats

机译:趋化因子CXCL13在大鼠骨癌疼痛发育中的作用及大鼠吗啡镇痛调控

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摘要

Chemokines are important regulators of immune, inflammatory, and neuronal responses in peripheral and central pain pathway. The aim of this study was to investigate whether chemokine (C-X-C motif) ligand 13 (CXCL13) and its receptor (C-X-C chemokine receptor type 5, CXCR5) involve in the development of bone cancer pain (BCP) and the regulation of morphine analgesia in rats. The change of pain behaviors in BCP rats were measured by testing paw withdrawal threshold (PWT). The levels of CXCL13, CXCR5 and signal pathway proteins (p-p38, p-ERK and p-AKT etc.) in the spinal cord were measured via western blots. The expression of CXCL13 and CXCR5 in spinal cord was increased in BCP rats. The BCP rats showed decrease of PWTs, which was relieved by CXCR5i. Intrathecally injection of murine recombinant CXCL13 (mrCXCL13) decreased the PWTs of BCP rats and opposed morphine-induced analgesia in BCP rats. In BCP rats, the signal pathway proteins (p38, ERK and AKT) in the spinal cord were activated. CXCL13 and morphine had contrary effect on the phosphorylation of these proteins. MrCXCL13 directly increased the levels of p-p38, p-ERK and p-AKT in BCP rats. However, morphine decreased the levels of these proteins in BCP rats. While blocking the activation of p-p38, p-ERK and p-AKT, morphine analgesia was enhanced. These results suggest CXCL13 participated in bone cancer pain and opposed morphine analgesia via p38, ERK and AKT pathways. It may be a target to enhance pain management in cancer pain patients. (C) 2019 IBRO. Published by Elsevier Ltd. All rights reserved.
机译:趋化因子是外周和中枢疼痛途径的免疫,炎症和神经元反应的重要调节因素。本研究的目的是研究趋化因子(CXC基序)配体13(CXC113)及其受体(CXC趋化因子受体类型5,CXCR5)是否涉及骨癌疼痛(BCP)的发育和大鼠吗啡镇痛的调节。通过测试爪子取出阈值(PWT)测量BCP大鼠疼痛行为的变化。通过蛋白质印迹测量脊髓中的CXCL13,CXCR5和信号途径蛋白(P-P38,P-ERK和P-AKT等)的水平。在BCP大鼠中增加了CXCL13和CXCR5在脊髓中的表达。 BCP大鼠显示PWT的降低,其通过CXCR5i缓解。鞘内注射鼠重组CXCL13(MRCXCL13)降低了BCP大鼠BCP大鼠的PWT,并在BCP大鼠中的镇痛。在BCP大鼠中,激活脊髓中的信号途径蛋白(P38,ERK和AKT)。 CXCL13和吗啡对这些蛋白质的磷酸化有相反的影响。 MRCXCL13在BCP大鼠中直接增加P-P38,P-ERK和P-AKT的水平。然而,吗啡在BCP大鼠中降低了这些蛋白质的水平。在阻断P-P38的激活时,P-ERK和P-AKT,增强了吗啡镇痛。这些结果表明CXCL13通过P38,ERK和AKT途径参与骨癌疼痛和反对吗啡镇痛。它可能是增强癌症疼痛患者疼痛管理的靶标。 (c)2019年IBRO。 elsevier有限公司出版。保留所有权利。

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  • 作者单位

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Dept Anesthesiol Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Dept Anesthesiol Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

    Zhengzhou Univ Dept Anesthesiol Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Sch Basic Med Sci Zhengzhou 450000 Henan Peoples R China;

    Zhengzhou Univ Sch Basic Med Sci Zhengzhou 450000 Henan Peoples R China;

    Zhengzhou Univ Dept Pain Management Affiliated Hosp 1 1 Jian She Dong Rd Zhengzhou 450052;

    Zhengzhou Univ Dept Anesthesiol Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

    Zhengzhou Univ Dept Anesthesiol Affiliated Hosp 1 Zhengzhou 450052 Henan Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 人体生理学;
  • 关键词

    CXCL13; cancer pain; morphine; signaling pathways; siRNA;

    机译:CXCL13;癌症疼痛;吗啡;信号通路;siRNA;

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