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自闭症和脆性 X 综合征中神经改变与基因型的关联:在因果建模中纳入感知表型。

Associating neural alterations and genotype in autism and fragile x syndrome: incorporating perceptual phenotypes in causal modeling.

机构信息

Perceptual Neuroscience Laboratory for Autism and Developmental Conditions, University of Montreal Center of Excellence for Pervasive Developmental Disorders (CETEDUM), Hôpital Rivière-des-Prairies, 7070 boulevard Perras, Montreal, Quebec, Canada.

出版信息

J Autism Dev Disord. 2010 Dec;40(12):1541-8. doi: 10.1007/s10803-010-1110-z.

Abstract

We have previously described (see companion paper, this issue) the utility of using perceptual signatures for defining and dissociating condition-specific neural functioning underlying early visual processes in autism and FXS. These perceptually-driven hypotheses are based on differential performance evidenced only at the earliest stages of visual information processing, mediated by local neural network functioning. In this paper, we first review how most large-scale neural models are unable to address atypical low-level perceptual functioning in autism, and then suggest how condition-specific, local neural endophenotypes (described in our companion paper) can be incorporated into causal models to infer target candidate gene or gene clusters that are implicated in autism's pathogenesis. The usefulness of such a translational research approach is discussed.

摘要

我们之前已经描述过(见本期的相关论文),使用感知特征来定义和区分自闭症和脆性 X 综合征中早期视觉过程的特定条件下的神经功能的有效性。这些基于感知的假设是基于仅在视觉信息处理的最早阶段表现出的差异性能,由局部神经网络功能介导。在本文中,我们首先回顾了大多数大规模神经模型如何无法解决自闭症中异常的低水平感知功能,然后提出了如何将特定于条件的局部神经内表型(在我们的相关论文中描述)纳入因果模型,以推断出与自闭症发病机制相关的候选靶基因或基因簇。讨论了这种转化研究方法的有用性。

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