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产前地西泮暴露对新生和幼鼠呼吸控制和单胺能系统的性别二态影响。

Sexually dimorphic effects of prenatal diazepam exposure on respiratory control and the monoaminergic system of neonate and young rats.

机构信息

Department of Animal Morphology and Physiology, FCAV - UNESP - São Paulo State University, Jaboticabal, SP, Brazil.

Department of Physiology, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, Al, Canada.

出版信息

Pflugers Arch. 2022 Nov;474(11):1185-1200. doi: 10.1007/s00424-022-02730-7. Epub 2022 Jul 25.

Abstract

Pregnancy is highly affected by anxiety disorders, which may be treated with benzodiazepines, especially diazepam (DZP), that can cross the placental barrier and interact with the fetal GABAergic system. We tested whether prenatal exposure to DZP promotes sex-specific postnatal changes in the respiratory control of rats. We evaluated ventilation ([Formula: see text]) and oxygen consumption ([Formula: see text] O) in resting conditions and under hypercapnia (7% CO) and hypoxia (10% O) in newborn [postnatal day (P) 0-1 and P12-13)] and young (P21-22) rats from mothers treated with DZP during pregnancy. We also analyzed brainstem monoamines at the same ages. DZP exposure had minimal effects on room air-breathing variables in females, but caused hypoventilation (drop in [Formula: see text]/[Formula: see text] O) in P12-13 males, lasting until P21-22. The hypercapnic ventilatory response was attenuated in P0-1 and P12-13 DZP-treated females mainly by a decrease in tidal volume (V), whereas males had a reduction in respiratory frequency (f) at P12-13. Minor changes were observed in hypoxia, but an attenuation in [Formula: see text] was seen in P12-13 males. In the female brainstem, DZP increased dopamine concentration and decreased 5-hydroxyindole-3-acetic acid (5-HIAA) and the 3,4-dihydroxyphenylacetic acid (DOPAC)/dopamine ratio at P0-1, and reduced DOPAC concentration at P12-13. In males, DZP decreased brainstem noradrenaline at P0-1. Our results demonstrate that prenatal DZP exposure reduces CO chemoreflex only in postnatal females and does not affect hypoxia-induced hyperventilation in both sexes. In addition, prenatal DZP alters brainstem monoamine concentrations throughout development differently in male and female rats.

摘要

妊娠受焦虑障碍的影响很大,焦虑障碍可以用苯二氮䓬类药物治疗,特别是地西泮(DZP),它可以穿过胎盘屏障并与胎儿 GABA 能系统相互作用。我们测试了产前暴露于 DZP 是否会促进大鼠出生后呼吸控制的性别特异性变化。我们评估了在休息状态下以及在新生(出生后第 0-1 天和第 12-13 天)和幼鼠(第 21-22 天)中,母体在怀孕期间接受 DZP 治疗时的通气([Formula: see text])和耗氧量([Formula: see text] O)在高碳酸血症(7% CO)和低氧血症(10% O)下的变化。我们还在同一时期分析了脑干单胺类物质。DZP 暴露对雌性的空气呼吸变量几乎没有影响,但在 P12-13 雄性中引起通气不足([Formula: see text]/[Formula: see text] O 下降),持续到 P21-22。在 P0-1 和 P12-13 接受 DZP 治疗的雌性中,高碳酸血症通气反应减弱主要是由于潮气量(V)减少,而雄性在 P12-13 时呼吸频率(f)降低。在低氧血症中观察到较小的变化,但在 P12-13 雄性中观察到[Formula: see text]减弱。在雌性脑干中,DZP 在 P0-1 时增加多巴胺浓度并降低 5-羟色胺-3-乙酸(5-HIAA)和 3,4-二羟基苯乙酸(DOPAC)/多巴胺比值,并在 P12-13 时降低 DOPAC 浓度。在雄性中,DZP 在 P0-1 时减少脑干去甲肾上腺素。我们的结果表明,产前 DZP 暴露仅在产后雌性中降低 CO 化学感受器反射,而不影响两性的缺氧性过度通气。此外,产前 DZP 在整个发育过程中以不同的方式改变雄性和雌性大鼠脑干单胺浓度。

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