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在幼鼠创伤性脑损伤后的急性期,丁丙诺啡对成年海马神经发生和行为结果的性别特异性影响。

Sex specific effects of buprenorphine on adult hippocampal neurogenesis and behavioral outcomes during the acute phase after pediatric traumatic brain injury in mice.

机构信息

Department of Natural Sciences, College of Arts, Sciences, and Letters, University of Michigan-Dearborn, 4901 Evergreen Rd, Dearborn, MI, 48128, USA.

Unit for Laboratory Animal Medicine, University of Michigan-Ann Arbor, 2800 Plymouth Rd, Ann Arbor, MI, 48109, USA.

出版信息

Neuropharmacology. 2024 Mar 1;245:109829. doi: 10.1016/j.neuropharm.2023.109829. Epub 2023 Dec 29.

Abstract

Traumatic brain injury (TBI) in children often causes cognitive and mental dysfunctions, as well as acute and chronic pain. Adult hippocampal neurogenesis plays a key role in cognition, depression, and pain. Adult hippocampal neurogenesis can be modulated by genetic and environmental factors, such as TBI and opioids. Buprenorphine (BPN), a semisynthetic opioid, is commonly used for pain management in children, however, the effects of BPN on adult hippocampal neurogenesis after pediatric TBI are still unclear. This study investigated the sex-specific effects of BPN on adult hippocampal neurogenesis during acute phase after pediatric TBI. Male and female littermates were randomized on postnatal day 20-21(P20-21) into Sham, TBI+saline and TBI+BPN groups. BPN was administered intraperitoneally to the TBI+BPN mice at 30 min after injury, and then every 6-12 h (h) for 2 days (d). Bromodeoxyuridine (BrdU) was administered intraperitoneally to all groups at 2, 4, 6, and 8-h post-injury. All outcomes were evaluated at 3-d post-BrdU administration. We found that TBI induced significant cognitive impairment, depression, and reduced adult hippocampal neurogenesis in both male and female mice, with more prominent effects in females. BPN significantly improved adult hippocampal neurogenesis and depression in males, but not in females. We further demonstrated that differential expressions of opioid receptors, transcription factors and neuroinflammatory markers at the neurogenic niche might be responsible for the differential effects of BPN in males and females. In conclusion, this study elucidates the effects of BPN on adult hippocampal neurogenesis and behavioral outcomes at the acute phase after pediatric TBI.

摘要

儿童创伤性脑损伤(TBI)常导致认知和精神功能障碍,以及急性和慢性疼痛。成人海马神经发生在认知、抑郁和疼痛中发挥关键作用。成人海马神经发生可受遗传和环境因素的调节,如 TBI 和阿片类药物。丁丙诺啡(BPN),一种半合成阿片类药物,常用于儿童疼痛管理,然而,BPN 对儿科 TBI 后成年海马神经发生的影响尚不清楚。本研究探讨了 BPN 在儿科 TBI 后急性期对成年海马神经发生的性别特异性影响。雄性和雌性同窝仔鼠在出生后第 20-21 天(P20-21)随机分为假手术、TBI+盐水和 TBI+BPN 组。TBI+BPN 组在损伤后 30 分钟内经腹腔给予 BPN,然后每 6-12 小时(h)给予 2 天(d)。所有组均在损伤后 2、4、6 和 8 小时给予腹腔注射溴脱氧尿苷(BrdU)。所有结果均在 BrdU 给药后 3 天评估。我们发现 TBI 导致雄性和雌性小鼠均出现明显的认知障碍、抑郁和成年海马神经发生减少,而雌性小鼠的影响更为显著。BPN 显著改善了雄性小鼠的成年海马神经发生和抑郁,但对雌性小鼠没有影响。我们进一步证明,神经发生龛中阿片受体、转录因子和神经炎症标志物的差异表达可能是 BPN 在雄性和雌性中产生差异作用的原因。总之,本研究阐明了 BPN 在儿科 TBI 后急性期对成年海马神经发生和行为结果的影响。

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