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丁丙诺啡对小鼠小儿创伤性脑损伤后行为、星形胶质细胞阿片受体表达和神经炎症的性别特异性影响。

Sex specific effects of buprenorphine on behavior, astrocytic opioid receptor expression and neuroinflammation after pediatric traumatic brain injury in mice.

作者信息

Hamood Yesmine, Abdullah Mauda, El Ghoul Hassan, Saad Nazeh, Dysko Robert C, Zhang Zhi

机构信息

Department of Natural Sciences, University of Michigan-Dearborn, Dearborn, MI, USA.

Unit for Laboratory Animal Medicine, University of Michigan-Ann Arbor, Ann Arbor, MI, USA.

出版信息

Brain Behav Immun Health. 2022 May 13;22:100469. doi: 10.1016/j.bbih.2022.100469. eCollection 2022 Jul.

Abstract

Children who suffered traumatic brain injury (TBI) often experience acute and chronic pain, which is linked to a poor quality of life. Buprenorphine (BPN) is commonly used to treat moderate to severe persistent pain in children, however, the efficacy and safety profile of BPN in the pediatric population is still inconclusive. This study investigated the sex-specific effects of BPN on body weight, motor coordination and strength, expression of opioid receptors in the white matter astrocytes, and neuroinflammation in a mouse impact acceleration model of pediatric TBI. Male and female littermates were randomized on postnatal day 20-21(P20-21) into Sham, TBI + saline and TBI + BPN groups. Mice in the TBI + saline and TBI + BPN groups underwent TBI, while the Sham group underwent anesthesia without injury. BPN (0.075 mg/kg) was administered to the TBI + BPN mice at 30 min after injury, and then every 6-12 h for 2 days. Mice in the TBI + saline group received the same amount of saline injections. The impact of BPN on body weight, motor function, opioid receptor expression, and neuroinflammation was evaluated at 1-day (d), 3-d and 7-d post-injury. We found that 1) TBI induced significant weight loss in both males and females. BPN treatment improved weight loss at 3-d post-injury in females. 2) TBI significantly impaired motor coordination and strength. BPN improved motor coordination and strength in both males and females at 1-d and 3-d post-injury. 3) TBI significantly decreased exploration activity at 1-d post-injury in males, and at 7-d post-injury in females, while BPN improved the exploration activity in females. 4) TBI significantly increased mRNA expression of mu-opioid receptors (MOR) at 7-d post-injury in males, but decreased mRNA expression of MOR at 1-d post-injury in females. BPN normalized MOR mRNA expression at 1-d post-injury in females. 5) MOR expression in astrocytes at corpus callosum significantly increased at 7-d post-injury in male TBI group, but significantly decreased at 1-d post-injury in female TBI group. BPN normalized MOR expression in both males and females. 6) TBI significantly increased the mRNA expression of TNF-α, IL-1β, IL-6 and iNOS. BPN decreased mRNA expression of iNOS, and increased mRNA expression of TGF-β1. In conclusion, this study elucidates the sex specific effects of BPN during the acute phase after pediatric TBI, which provides the rationale to assess potential effects of BPN on chronic pathological progressions after pediatric TBI in both males and females.

摘要

遭受创伤性脑损伤(TBI)的儿童常经历急性和慢性疼痛,这与生活质量差有关。丁丙诺啡(BPN)常用于治疗儿童中度至重度持续性疼痛,然而,BPN在儿科人群中的疗效和安全性仍不明确。本研究在儿科TBI小鼠撞击加速模型中,研究了BPN对体重、运动协调和力量、白质星形胶质细胞中阿片受体表达以及神经炎症的性别特异性影响。将出生后第20 - 21天(P20 - 21)的雄性和雌性同窝幼崽随机分为假手术组、TBI + 生理盐水组和TBI + BPN组。TBI + 生理盐水组和TBI + BPN组的小鼠接受TBI,而假手术组接受无损伤的麻醉。在损伤后30分钟给TBI + BPN组小鼠注射BPN(0.075 mg/kg),然后每6 - 12小时注射一次,持续2天。TBI + 生理盐水组的小鼠接受等量的生理盐水注射。在损伤后1天(d)、3天和7天评估BPN对体重、运动功能、阿片受体表达和神经炎症的影响。我们发现:1)TBI导致雄性和雌性小鼠体重显著下降。BPN治疗改善了雌性小鼠损伤后3天的体重减轻。2)TBI显著损害运动协调和力量。BPN改善了雄性和雌性小鼠损伤后1天和3天的运动协调和力量。3)TBI显著降低了雄性小鼠损伤后1天和雌性小鼠损伤后7天的探索活动,而BPN改善了雌性小鼠的探索活动。4)TBI显著增加了雄性小鼠损伤后7天μ-阿片受体(MOR)的mRNA表达,但降低了雌性小鼠损伤后1天MOR的mRNA表达。BPN使雌性小鼠损伤后1天的MOR mRNA表达恢复正常。5)胼胝体星形胶质细胞中的MOR表达在雄性TBI组损伤后7天显著增加,但在雌性TBI组损伤后1天显著降低。BPN使雄性和雌性小鼠的MOR表达恢复正常。6)TBI显著增加了TNF-α、IL-1β、IL-6和iNOS的mRNA表达。BPN降低了iNOS的mRNA表达,并增加了TGF-β1的mRNA表达。总之,本研究阐明了儿科TBI急性期BPN的性别特异性影响,这为评估BPN对儿科TBI后男性和女性慢性病理进展的潜在影响提供了理论依据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b826/9127176/fd53160c249a/gr1.jpg

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