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产前或青春期尼古丁暴露单独或相继对大鼠脑区产生的永久性、性别选择性影响:6月龄时胆碱能和血清素能突触功能、细胞信号传导以及神经细胞数量和大小的指标

Permanent, sex-selective effects of prenatal or adolescent nicotine exposure, separately or sequentially, in rat brain regions: indices of cholinergic and serotonergic synaptic function, cell signaling, and neural cell number and size at 6 months of age.

作者信息

Slotkin Theodore A, MacKillop Emiko A, Rudder Charles L, Ryde Ian T, Tate Charlotte A, Seidler Frederic J

机构信息

Department of Pharmacology and Cancer Biology, Duke University Medical Center, Durham, NC 27710, USA.

出版信息

Neuropsychopharmacology. 2007 May;32(5):1082-97. doi: 10.1038/sj.npp.1301231. Epub 2006 Oct 18.

Abstract

Nicotine is a neuroteratogen that disrupts neurodevelopment and synaptic function, with vulnerability extending into adolescence. We assessed the permanence of effects in rats on indices of neural cell number and size, and on acetylcholine and serotonin (5HT) systems, conducting assessments at 6 months of age, after prenatal nicotine exposure, adolescent exposure, or sequential exposure in both periods. For prenatal nicotine, indices of cell number and size showed few abnormalities by 6 months, but there were persistent deficits in cerebrocortical choline acetyltransferase activity and hemicholinium-3 binding to the presynaptic choline transporter, a pattern consistent with cholinergic hypoactivity; these effects were more prominent in males than females. The expression of 5HT receptors also showed permanent effects in males, with suppression of the 5HT(1A) subtype and upregulation of 5HT(2) receptors. In addition, cell signaling through adenylyl cyclase showed heterologous uncoupling of neurotransmitter responses. Nicotine exposure in adolescence produced lasting effects that were similar to those of prenatal nicotine. However, when animals were exposed to prenatal nicotine and received nicotine subsequently in adolescence, the adverse effects then extended to females, whereas the net effect in males was similar to that of prenatal nicotine by itself. Our results indicate that prenatal or adolescent nicotine exposure evoke permanent changes in synaptic function that transcend the recovery of less-sensitive indices of structural damage; further, prenatal exposure sensitizes females to the subsequent adverse effects of adolescent nicotine, thus creating a population that may be especially vulnerable to the lasting behavioral consequences of nicotine intake in adolescence.

摘要

尼古丁是一种神经致畸剂,会干扰神经发育和突触功能,这种易损性会持续到青春期。我们评估了大鼠在产前尼古丁暴露、青春期暴露或两个时期连续暴露后,于6月龄时对神经细胞数量和大小指标以及乙酰胆碱和血清素(5-羟色胺,5HT)系统的影响的持久性。对于产前尼古丁暴露,到6个月时细胞数量和大小指标几乎没有异常,但脑皮质胆碱乙酰转移酶活性以及半胱氨酸-3与突触前胆碱转运体的结合存在持续缺陷,这一模式与胆碱能活性不足一致;这些影响在雄性中比雌性更明显。5HT受体的表达在雄性中也显示出永久性影响,5HT(1A)亚型受到抑制,5HT(2)受体上调。此外,通过腺苷酸环化酶的细胞信号传导显示神经递质反应存在异源解偶联。青春期尼古丁暴露产生的持久影响与产前尼古丁暴露相似。然而,当动物在产前暴露于尼古丁并在青春期随后接触尼古丁时,不良影响随后扩展到雌性,而雄性的总体影响与单独产前尼古丁暴露时相似。我们的结果表明,产前或青春期尼古丁暴露会引起突触功能的永久性变化,这种变化超越了结构损伤较不敏感指标的恢复;此外,产前暴露使雌性对青春期尼古丁的后续不良影响敏感,从而形成一个可能特别容易受到青春期尼古丁摄入持久行为后果影响的群体。

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