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婴儿期促红细胞生成素和褪黑素鸡尾酒疗法可恢复早产儿脑损伤成年大鼠的步态。

Infantile Cocktail of Erythropoietin and Melatonin Restores Gait in Adult Rats with Preterm Brain Injury.

机构信息

Department of Neurosurgery, Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.

Department of Pediatrics, Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.

出版信息

Dev Neurosci. 2022;44(4-5):266-276. doi: 10.1159/000524394. Epub 2022 Mar 31.

Abstract

Cerebral palsy (CP) is the most common cause of physical disability for children worldwide. Many infants and toddlers are not diagnosed with CP until they fail to achieve obvious motor milestones. Currently, there are no effective pharmacologic interventions available for infants and toddlers to substantially improve their trajectory of neurodevelopment. Because children with CP from preterm birth also exhibit a sustained immune system hyper-reactivity, we hypothesized that neuro-immunomodulation with a regimen of repurposed endogenous neurorestorative medications, erythropoietin (EPO) and melatonin (MLT), could improve this trajectory. Thus, we administered EPO + MLT to rats with CP during human infant-toddler equivalency to determine whether we could influence gait patterns in mature animals. After a prenatal injury on embryonic day 18 (E18) that mimics chorioamnionitis at ∼25 weeks human gestation, rat pups were born and raised with their dam. Beginning on postnatal day 15 (P15), equivalent to human infant ∼1 year, rats were randomized to receive either a regimen of EPO + MLT or vehicle (sterile saline) through P20. Gait was assessed in young adult rats at P30 using computerized digital gait analyses including videography on a treadmill. Results indicate that gait metrics of young adult rats treated with an infantile cocktail of EPO + MLT were restored compared to vehicle-treated rats (p < 0.05) and similar to sham controls. These results provide reassuring evidence that pharmacological interventions may be beneficial to infants and toddlers who are diagnosed with CP well after the traditional neonatal window of intervention.

摘要

脑瘫(CP)是全球儿童最常见的身体残疾原因。许多婴儿和幼儿直到未能达到明显的运动里程碑时才被诊断出患有 CP。目前,对于婴儿和幼儿来说,没有有效的药物干预措施可以显著改善他们的神经发育轨迹。由于早产儿 CP 患儿还表现出持续的免疫系统过度反应,我们假设用重新利用的内源性神经修复药物,促红细胞生成素(EPO)和褪黑素(MLT)的神经免疫调节方案,可以改善这种轨迹。因此,我们在人类婴儿-幼儿等效阶段向 CP 大鼠给予 EPO+MLT,以确定我们是否可以影响成熟动物的步态模式。在模仿人类妊娠 25 周左右绒毛膜羊膜炎的胚胎 18 日(E18)产前损伤后,大鼠幼崽出生并与母鼠一起饲养。从出生后第 15 天(P15)开始,相当于人类婴儿约 1 岁,大鼠随机接受 EPO+MLT 方案或载体(无菌生理盐水)治疗至 P20。在 P30 时,使用计算机数字步态分析(包括在跑步机上的录像)评估幼鼠的步态。结果表明,接受婴儿期 EPO+MLT 鸡尾酒治疗的幼鼠的步态指标与接受载体治疗的大鼠相比得到了恢复(p<0.05),并且与假手术对照组相似。这些结果提供了令人放心的证据,表明药物干预措施可能对被诊断出患有 CP 的婴儿和幼儿有益,尽管已经错过了传统的新生儿干预窗口期。

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