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发育过程中接触甲基苯丙胺的神经行为影响。

Neurobehavioral Effects from Developmental Methamphetamine Exposure.

作者信息

Jablonski Sarah A, Williams Michael T, Vorhees Charles V

机构信息

Division of Neurology, Cincinnati Children's Hospital Medical Center, 3333 Burnet Ave., R-1447, Cincinnati, OH, 45229-3039, USA.

Division of Neurology, Cincinnati Children's Hospital Medical Center and Department of Pediatrics, University of Cincinnati College of Medicine, 45229, Cincinnati, OH, USA.

出版信息

Curr Top Behav Neurosci. 2016;29:183-230. doi: 10.1007/7854_2015_405.

Abstract

Intrauterine methamphetamine exposure adversely affects the neurofunctional profile of exposed children, leading to a variety of higher order cognitive deficits, such as decreased attention, reduced working-memory capability, behavioral dysregulation, and spatial memory impairments (Kiblawi et al. in J Dev Behav Pediatr 34:31-37, 2013; Piper et al. in Pharmacol Biochem Behav 98:432-439 2011; Roussotte et al. in Neuroimage 54:3067-3075, 2011; Twomey et al. in Am J Orthopsychiatry 83:64-72, 2013). In animal models of developmental methamphetamine, both neuroanatomical and behavioral outcomes critically depend on the timing of methamphetamine administration. Methamphetamine exposure during the third trimester human equivalent period of brain development results in well-defined and persistent wayfinding and spatial navigation deficits in rodents (Vorhees et al. in Neurotoxicol Teratol 27:117-134, 2005, Vorhees et al. in Int J Dev Neurosci 26:599-610, 2008; Vorhees et al. in Int J Dev Neurosci 27:289-298, 2009; Williams et al. in Psychopharmacology (Berl) 168:329-338, 2003b), whereas drug delivery during the first and second trimester equivalents produces no such effect (Acuff-Smith et al. in Neurotoxicol Teratol 18:199-215, 1996; Schutova et al. in Physiol Res 58:741-750, 2009a; Slamberova et al. in Naunyn Schmiedebergs Arch Pharmacol 380:109-114, 2009, Slamberova et al. in Physiol Res 63:S547-S558, 2014b). In this review, we examine the impact of developmental methamphetamine on emerging neural circuitry, neurotransmission, receptor changes, and behavioral outcomes in animal models. The review is organized by type of effects and timing of drug exposure (prenatal only, pre- and neonatal, and neonatal only). The findings elucidate functional patterns of interconnected brain structures (e.g., frontal cortex and striatum) and neurotransmitters (e.g., dopamine and serotonin) involved in methamphetamine-induced developmental neurotoxicity.

摘要

子宫内甲基苯丙胺暴露会对受暴露儿童的神经功能状况产生不利影响,导致多种高级认知缺陷,如注意力下降、工作记忆能力降低、行为失调以及空间记忆受损(Kiblawi等人,《发育与行为儿科学杂志》34:31 - 37,2013年;Piper等人,《药理学与生物化学行为》98:432 - 439,2011年;Roussotte等人,《神经影像学》54:3067 - 3075,2011年;Twomey等人,《美国儿童与青少年精神病学杂志》83:64 - 72,2013年)。在甲基苯丙胺发育的动物模型中,神经解剖学和行为学结果都严重依赖于甲基苯丙胺给药的时间。在人类大脑发育的第三个月等效期接触甲基苯丙胺会导致啮齿动物出现明确且持续的寻路和空间导航缺陷(Vorhees等人,《神经毒理学与致畸学》27:117 - 134,2005年;Vorhees等人,《国际发育神经科学杂志》26:599 - 610,2008年;Vorhees等人,《国际发育神经科学杂志》27:289 - 298,2009年;Williams等人,《精神药理学》168:329 - 338,2003b),而在第一个和第二个月等效期给药则不会产生这种影响(Acuff - Smith等人,《神经毒理学与致畸学》18:199 - 215,1996年;Schutova等人,《生理学研究》58:741 - 750,2009a;Slamberova等人,《瑙恩 - 席米德贝格药理学文献》380:109 - 114,2009年;Slamberova等人,《生理学研究》63:S547 - S558,2014b)。在本综述中,我们研究了发育性甲基苯丙胺对动物模型中新兴神经回路、神经传递、受体变化和行为结果的影响。该综述按效应类型和药物暴露时间(仅产前、产前和新生儿期、仅新生儿期)进行组织。这些发现阐明了参与甲基苯丙胺诱导的发育性神经毒性的相互连接的脑结构(如额叶皮质和纹状体)和神经递质(如多巴胺和血清素)的功能模式。

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