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早产对豚鼠神经活性甾体浓度的影响。

Changes in neuroactive steroid concentrations after preterm delivery in the Guinea pig.

机构信息

1Mothers and Babies Research Centre, Hunter Medical Research Institute, Newcastle, New South Wales, Australia.

出版信息

Reprod Sci. 2013 Nov;20(11):1365-75. doi: 10.1177/1933719113485295. Epub 2013 Apr 12.

Abstract

BACKGROUND

Preterm birth is a major cause of neurodevelopmental disorders. Allopregnanolone, a key metabolite of progesterone, has neuroprotective and developmental effects in the brain. The objectives of this study were to measure the neuroactive steroid concentrations following preterm delivery in a neonatal guinea pig model and assess the potential for postnatal progesterone replacement therapy to affect neuroactive steroid brain and plasma concentrations in preterm neonates.

METHODS

Preterm (62-63 days) and term (69 days) guinea pig pups were delivered by cesarean section and tissue was collected at 24 hours. Plasma progesterone, cortisol, allopregnanolone, and brain allopregnanolone concentrations were measured by immunoassay. Brain 5α-reductase (5αR) expression was determined by Western blot. Neurodevelopmental maturity of preterm neonates was assessed by immunohistochemistry staining for myelination, glial cells, and neurons.

RESULTS

Brain allopregnanolone concentrations were significantly reduced after birth in both preterm and term neonates. Postnatal progesterone treatment in preterm neonates increased brain and plasma allopregnanolone concentrations. Preterm neonates had reduced myelination, low birth weight, and high mortality compared to term neonates. Brain 5αR expression was also significantly reduced in neonates compared to fetal expression.

CONCLUSIONS

Delivery results in a loss of neuroactive steroid concentrations resulting in a premature reduction in brain allopregnanolone in preterm neonates. Postnatal progesterone therapy reestablished neuroactive steroid levels in preterm brains, a finding that has implications for postnatal growth following preterm birth that occurs at a time of neurodevelopmental immaturity.

摘要

背景

早产是神经发育障碍的主要原因。孕酮的关键代谢物别孕烯醇酮在大脑中具有神经保护和发育作用。本研究的目的是测量早产新生儿模型中早产分娩后神经活性类固醇的浓度,并评估产后孕激素替代疗法对早产新生儿大脑和血浆中神经活性类固醇浓度的潜在影响。

方法

通过剖腹产分娩早产(62-63 天)和足月(69 天)豚鼠幼崽,并在 24 小时收集组织。通过免疫测定法测量血浆孕酮、皮质醇、别孕烯醇酮和大脑别孕烯醇酮浓度。通过 Western blot 测定脑 5α-还原酶(5αR)表达。通过髓鞘、神经胶质细胞和神经元免疫组织化学染色评估早产新生儿的神经发育成熟度。

结果

在足月和早产新生儿出生后,大脑别孕烯醇酮浓度均显著降低。在早产新生儿中进行产后孕激素治疗可增加大脑和血浆中的别孕烯醇酮浓度。与足月新生儿相比,早产新生儿的髓鞘形成减少、出生体重低且死亡率高。与胎儿表达相比,新生儿的脑 5αR 表达也显著降低。

结论

分娩导致神经活性类固醇浓度丧失,导致早产新生儿大脑中别孕烯醇酮过早减少。产后孕激素治疗恢复了早产婴儿大脑中的神经活性类固醇水平,这一发现对早产儿出生后神经发育不成熟时期的产后生长具有重要意义。

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