Department of Physiology and Neurobiology, Geisel school of Medicine at Dartmouth, Lebanon, NH, 03756, USA.
Department of Molecular and Systems Biology, Geisel school of Medicine at Dartmouth, Lebanon, NH, 03756, USA.
J Physiol. 2018 Dec;596(23):5977-5991. doi: 10.1113/JP275885. Epub 2018 Jul 15.
Sudden infant death syndrome (SIDS) is one of the leading causes of death during the first year of life and abnormalities linked to serotonin (5-HT) have been identified in many SIDS cases. Cigarette smoking and associated exogenous stressors, e.g. developmental nicotine exposure, may compound these serotonergic defects and any associated defects in cardiorespiratory function. Using neonatal rodent pups subjected to medullary 5-HT deficiency and perinatal nicotine exposure, we examined the impact of this interplay of factors on the neonates' ability to autoresuscitate at specific ages. In perinatal nicotine-exposed 5-HT deficient pups, impaired autoresuscitation along with significantly delayed post-anoxic recovery of normal breathing and heart rate was observed at postnatal day 10 (P10). We found that the interaction between 5-HT deficiency and perinatal nicotine exposure can significantly increase pups' vulnerability to environmental stressors and exacerbate defects in cardiorespiratory protective reflexes to repetitive anoxia during the development period.
Cigarette smoking during pregnancy increases the risk of sudden infant death syndrome (SIDS), and nicotine replacements, a key ingredient of cigarettes, have been recently prescribed to women who wish to quit smoking during their pregnancy. Serotonin (5-HT) abnormalities have been consistently identified in many SIDS cases. Here we investigated the effects of perinatal nicotine exposure in mild 5-HT deficiency rat neonates on autoresuscitation, a protective cardiorespiratory reflex. The mild 5-HT deficiency was induced by a maternal tryptophan-deficient diet, and nicotine was delivered from embryonic day (E) 4 to postnatal day (P) 10 at 6 mg kg day through an osmotic pump. In P10 rats, nicotine exposure exacerbates autoresuscitation failure (mortality) in mildly 5-HT-deficient rats to a greater extent than in controls (P = 0.029). The recovery of eupnoea and heart rate to baseline values following repetitive anoxic events (which elicit an apnoea accompanied by a bradycardia) is significantly delayed in 5-HT-deficient rats treated with nicotine, making them more susceptible to failure of autoresuscitation (eupnoea recovery: P = 0.0053; heart rate recovery: P = < 0.0001). Neither 5-HT deficiency nor nicotine exposure alone appears to affect the ability to autoresuscitate significantly when compared among the four treatments. The increased vulnerability to environmental stressors, e.g. severe hypoxia, asphyxia, or anoxia, in these nicotine-exposed 5-HT-deficient neonates during postnatal developmental period is evident.
婴儿猝死综合征(SIDS)是婴儿期死亡的主要原因之一,许多 SIDS 病例中发现与 5-羟色胺(5-HT)相关的异常。吸烟和相关的外源性应激源,例如发育性尼古丁暴露,可能会使这些 5-羟色胺能缺陷以及任何相关的心肺功能缺陷更加复杂。使用接受延髓 5-HT 缺乏和围产期尼古丁暴露的新生啮齿动物幼仔,我们研究了这些因素相互作用对新生动物在特定年龄自主复苏能力的影响。在围产期尼古丁暴露的 5-HT 缺乏幼仔中,在出生后第 10 天(P10)观察到自主复苏受损,以及正常呼吸和心率的缺氧后恢复明显延迟。我们发现,5-HT 缺乏与围产期尼古丁暴露的相互作用可显著增加幼仔对环境应激源的易感性,并在发育期间加剧反复缺氧时对心肺保护性反射的缺陷。
怀孕期间吸烟会增加婴儿猝死综合征(SIDS)的风险,最近已将香烟的主要成分尼古丁替代品开给希望在怀孕期间戒烟的女性。许多 SIDS 病例中均发现 5-羟色胺(5-HT)异常。在这里,我们研究了围产期尼古丁暴露对轻度 5-HT 缺乏新生大鼠自主复苏的影响,自主复苏是一种保护性心肺反射。轻度 5-HT 缺乏是通过母体色氨酸缺乏饮食诱导的,从胚胎期第 4 天(E4)到出生后第 10 天(P10),通过渗透泵以 6mgkg 天的剂量给予尼古丁。在 P10 大鼠中,与对照组相比,尼古丁暴露使轻度 5-HT 缺乏大鼠的自主复苏失败(死亡率)恶化程度更大(P=0.029)。与对照组相比,接受尼古丁治疗的 5-HT 缺乏大鼠在重复缺氧事件后(引起伴有心动过缓的呼吸暂停)的 eupnoea 和心率恢复至基线值的时间明显延迟,使它们更容易发生自主复苏失败(eupnoea 恢复:P=0.0053;心率恢复:P<0.0001)。与四种处理方式相比,5-HT 缺乏或尼古丁暴露单独出现时,均不会明显影响自主复苏的能力。在出生后发育期间,这些暴露于尼古丁的 5-HT 缺乏新生动物对环境应激源(例如严重缺氧、窒息或缺氧)的易感性增加是显而易见的。
