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自闭症谱系障碍中的眼球跳动异常表明小脑和脑干存在功能障碍。

Saccadic eye movement abnormalities in autism spectrum disorder indicate dysfunctions in cerebellum and brainstem.

作者信息

Schmitt Lauren M, Cook Edwin H, Sweeney John A, Mosconi Matthew W

机构信息

Center for Autism and Developmental Disabilities, University of Texas Southwestern, 5323 Harry Hines Blvd, Dallas, TX 75390-9086 USA.

Department of Psychiatry, University of Illinois at Chicago, 1747 W. Roosevelt Rd (MC 747), Chicago, IL 60608 USA.

出版信息

Mol Autism. 2014 Sep 16;5(1):47. doi: 10.1186/2040-2392-5-47. eCollection 2014.

Abstract

BACKGROUND

Individuals with autism spectrum disorder (ASD) show atypical scan paths during social interaction and when viewing faces, and recent evidence suggests that they also show abnormal saccadic eye movement dynamics and accuracy when viewing less complex and non-social stimuli. Eye movements are a uniquely promising target for studies of ASD as their spatial and temporal characteristics can be measured precisely and the brain circuits supporting them are well-defined. Control of saccade metrics is supported by discrete circuits within the cerebellum and brainstem - two brain regions implicated in magnetic resonance (MR) morphometry and histopathological studies of ASD. The functional integrity of these distinct brain systems can be examined by evaluating different parameters of visually-guided saccades.

METHODS

A total of 65 participants with ASD and 43 healthy controls, matched on age (between 6 and 44-years-old), gender and nonverbal IQ made saccades to peripheral targets. To examine the influence of attentional processes, blocked gap and overlap trials were presented. We examined saccade latency, accuracy and dynamics, as well as the trial-to-trial variability of participants' performance.

RESULTS

Saccades of individuals with ASD were characterized by reduced accuracy, elevated variability in accuracy across trials, and reduced peak velocity and prolonged duration. In addition, their saccades took longer to accelerate to peak velocity, with no alteration in the duration of saccade deceleration. Gap/overlap effects on saccade latencies were similar across groups, suggesting that visual orienting and attention systems are relatively spared in ASD. Age-related changes did not differ across groups.

CONCLUSIONS

Deficits precisely and consistently directing eye movements suggest impairment in the error-reducing function of the cerebellum in ASD. Atypical increases in the duration of movement acceleration combined with lower peak saccade velocities implicate pontine nuclei, specifically suggesting reduced excitatory activity in burst cells that drive saccades relative to inhibitory activity in omnipause cells that maintain stable fixation. Thus, our findings suggest that both cerebellar and brainstem abnormalities contribute to altered sensorimotor control in ASD.

摘要

背景

自闭症谱系障碍(ASD)患者在社交互动和观察面部时表现出非典型的注视路径,最近的证据表明,他们在观察不太复杂的非社交刺激时,也表现出异常的扫视眼动动力学和准确性。眼动是ASD研究中一个特别有前景的目标,因为它们的空间和时间特征可以精确测量,并且支持眼动的脑回路也已明确。小脑和脑干内的离散回路支持对扫视指标的控制——这两个脑区在ASD的磁共振(MR)形态测量和组织病理学研究中均有涉及。通过评估视觉引导扫视的不同参数,可以检查这些不同脑系统的功能完整性。

方法

共有65名ASD患者和43名健康对照者参与研究,他们在年龄(6至44岁之间)、性别和非言语智商方面相匹配,向周边目标进行扫视。为了检查注意力过程的影响,进行了间隔和重叠试验。我们检查了扫视潜伏期、准确性和动力学,以及参与者表现的试验间变异性。

结果

ASD患者的扫视具有准确性降低、试验间准确性变异性升高、峰值速度降低和持续时间延长的特点。此外,他们的扫视加速到峰值速度所需的时间更长,扫视减速的持续时间没有改变。两组之间间隙/重叠对扫视潜伏期的影响相似,这表明ASD患者的视觉定向和注意力系统相对未受影响。各年龄组之间与年龄相关的变化没有差异。

结论

精确且一致地控制眼动的缺陷表明,ASD患者小脑的误差减少功能受损。运动加速持续时间的非典型增加与较低的扫视峰值速度相结合,提示脑桥核受累,具体表明驱动扫视的爆发细胞中的兴奋性活动相对于维持稳定注视的全暂停细胞中的抑制性活动降低。因此,我们的研究结果表明,小脑和脑干异常均导致ASD患者感觉运动控制改变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3134/4233053/6cd72c649c66/13229_2014_144_Fig1_HTML.jpg

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