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Translational Analysis of Effects of Prenatal Cocaine Exposure on Human Infant Cries and Rat Pup Ultrasonic Vocalizations

机译:产前可卡因暴露对婴儿啼哭和大鼠幼犬超声发声影响的转化分析

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摘要

Spectral and temporal features of human infant crying may detect neurobehavioral effects of prenatal cocaine exposure (PCE). Finding comparable measures of rodent ultrasonic vocalizations (USVs) would promote translational analyses by controlling the effects of correlated variables that confound human studies. To this end, two studies examined the sensitivity of similar acoustic structures in human infant and rat pup vocalizations to effects of PCE. In Study 1, cry sounds of 107 one month-old infants were spectrum analyzed to create a novel set of measures and to detect the presence of hyperphonation - a qualitative shift to an atypically high fundamental frequency (basic pitch) associated with neurobehavioral insult. Infants with PCE were compared to infants with prenatal polydrug-exposure (PPE) without cocaine and with infants in a standard comparison (SC) group with no prenatal drug exposure. In Study 2, USVs of 118 five day-old rat pups with either PCE, prenatal saline exposure or no prenatal exposures were spectrum analyzed to detect the presence of frequency shifts – acoustic features that have a frequency waveform similar to that of hyperphonation. Results of study 1 showed PCE had two sets of sex-dependent effects on human infants: PCE males had higher pitched cries with more dysphonation (turbulence); PCE females had longer pauses between fewer cry sounds that were of lower amplitude than comparison groups. PCE and PPE infants had more cries with hyperphonation than SC infants. In study 2, PCE pups had a greater percentage of USVs with shift in the acoustic structure than pups in the two control groups. As such, the novel measures of human infant crying and rat pup USVs were sensitive to effects of PCE. These studies provide the first known translational analysis of similar acoustic structures of vocalizations in two species to detect adverse effects of prenatal drug exposure.
机译:人类婴儿啼哭的频谱和时间特征可能检测出产前可卡因暴露(PCE)的神经行为影响。寻找啮齿类动物超声发声(USV)的可比较方法,可以通过控制混淆人类研究的相关变量的作用来促进翻译分析。为此,两项研究检查了人类婴儿和大鼠幼仔发声中类似声音结构对PCE影响的敏感性。在研究1中,对107个1个月大婴儿的哭声进行了频谱分析,以创建一套新颖的措施并检测超音的存在-一种向与神经行为侮辱相关的非典型高基频(基本音高)的定性转变。将具有PCE的婴儿与没有可卡因的产前多药暴露(PPE)婴儿和没有产前药物暴露的标准比较(SC)组中的婴儿进行了比较。在研究2中,对118只5日龄幼崽,有PCE,产前盐水暴露或无产前暴露的USV进行了频谱分析,以检测频移的存在-声学特征的频率波形与高音相似。研究1的结果表明,PCE对人类婴儿具有两套性别依赖性效应:PCE男性的哭声更高,吸音障碍(湍流)更多;与对照组相比,PCE女性在较少的哭声之间有较长的停顿时间,而哭声的幅度较低。与SC婴儿相比,PCE和PPE婴儿的高音哭声更高。在研究2中,与两个对照组中的幼崽相比,PCE幼崽的声音结构发生变化的USV百分比更高。因此,人类婴儿哭泣和大鼠幼仔USV的新措施对PCE的影响很敏感。这些研究为两个物种中相似的发声声学结构提供了第一个已知的翻译分析,以检测产前药物暴露的不利影响。

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