Parsing ASD Heterogeneity: Neuroendophenotypes of Social Attention and Sensory Responsivity
解析 ASD 异质性:社会注意力和感觉反应的神经内表型
基本信息
- 批准号:10412022
- 负责人:
- 金额:$ 72.6万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2018
- 资助国家:美国
- 起止时间:2018-08-01 至 2024-05-31
- 项目状态:已结题
- 来源:
- 关键词:AffectBehavioralBiological AssayBiological MarkersBrainChildhoodClinicalDataData AnalyticsData SetDevelopmentDiagnosisDimensionsElectroencephalographyEtiologyFemaleFosteringFunctional Magnetic Resonance ImagingFundingGenderGeneticGenetic PolymorphismGenetic Predisposition to DiseaseGenetic RiskGenomic approachGenotypeGoalsHeterogeneityHumanImageImpairmentIndividualIndividual DifferencesLinkMagnetic Resonance ImagingMapsMeasuresMotivationNational Institute of Mental HealthOutcomePatternPersonsPhenotypePopulationPropertyProtocols documentationPsychiatryReproducibilityResearchResearch Domain CriteriaResolutionRestRewardsRiskSamplingScanningSensorimotor functionsSensorySeveritiesSex DifferencesSiteSocial InteractionStimulusSubgroupSymptomsTranslational ResearchWorkYouthadolescent with autism spectrum disorderanalytical methodautism spectrum disorderbehavioral phenotypingbrain basedcohortcomorbidityconnectomeefficacious interventionendophenotypegenetic variantimaging geneticsimaging modalityindividuals with autism spectrum disorderinnovationinterestlarge datasetsmaleneuralneural circuitneurobiological mechanismneuroimagingneuromechanismnovelnovel strategiespersonalized interventionprecision medicinerepetitive behaviorresponserisk variantsensory stimulussexsocialsocial attentionsocial communicationsymptomatologytranslational potentialvirtual
项目摘要
PROJECT DESCRIPTION
Despite the tremendous variability observed across individuals diagnosed with Autism Spectrum Disorder
(ASD), most research to date has treated ASD as a unitary condition, comparing individuals with ASD to
neurotypical controls. This approach has hindered our progress in unraveling the neurobiological mechanisms
that give rise to ASD symptomatology and it also undermines the potential of translational research to
contribute to `precision medicine' in ASD. In this project, we take a critical step toward dissecting the significant
heterogeneity observed in ASD by combining state-of-the-art imaging methods, novel approaches to account
for genetic susceptibility, and a deep phenotypic characterization of a large and unique sample of males and
females with ASD that we curated as part of our recently renewed ACE Network (MH100028). Capitalizing on
the comprehensive assays already collected in this cohort (i.e., phenotyping, genotyping, MRI, EEG) and our
involvement in the Human Connectome Project - Development (MH109589), here we will collect and analyze a
rich dataset of brain-based measures of unparalleled resolution and quality in order to characterize individual
differences in brain network properties and examine how these relate to a vast phenotypic battery of measures
tapping into key domains of interest. Using resting-state fMRI and innovative fMRI activation tasks as neural
assays of social and sensory responsivity, we will examine how functional connectivity and brain responses in
associated neural circuits co-vary within and between individuals in order to determine how atypical reactivity
to sensory stimuli impacts neural processing of socially relevant stimuli, and assess how distinct neural
endophenotypes of social and sensory responsivity relate to altered functional connectivity and behavioral
phenotypes. Building upon our prior imaging-genetics work, we will also examine how polygenic risk, and risk
genetic variants on ASD-associated polymorphisms, influence brain function, connectivity, as well as core ASD
symptoms. Our overarching hypothesis is that both distinct and shared neuroendophenotypes will be identified
across our sample based on different brain function and connectivity metrics and that these will map onto
varying dimensions of social and sensory atypicalities manifested at the neural and behavioral level. We further
expect that higher polygenic risk will predict increasingly aberrant patterns of brain activity, connectivity, and
overall symptom severity, whereas genetic variance on ASD-associated polymorphisms will selectively
modulate brain function and connectivity in brain circuits where these ASD risk genes are expressed. By
employing (a) cutting-edge imaging methods to examine brain function and connectivity, (b) innovative
paradigms to relate social attention and motivation to sensory processing atypicalities, (c) novel approaches to
integrate genetic risk with neural and behavioral phenotypes, and (d) sophisticated data-analytic strategies to
sensibly stratify our ASD sample, this research will further our understanding of the neural mechanisms
underlying heterogeneity in ASD and ultimately inform more personalized and efficacious interventions.
项目描述
尽管在被诊断患有自闭症谱系障碍的个体中观察到巨大的变异性,
(ASD)迄今为止,大多数研究都将ASD视为一种单一的疾病,将ASD患者与
神经型对照。这种方法阻碍了我们在揭示神经生物学机制方面的进展
这导致了ASD的出现,它也破坏了转化研究的潜力,
有助于自闭症患者的“精准医疗”。在这个项目中,我们朝着解剖重要的一步迈出了关键的一步。
通过结合最先进的成像方法在ASD中观察到的异质性,
遗传易感性,以及对大量独特的男性样本进行深入的表型表征,
我们最近更新的ACE网络(MH 100028)的一部分。充分利用
已经在该群组中收集的综合测定(即,表型分型、基因分型、MRI、EEG)和我们的
参与人类连接组项目-开发(MH 109589),在这里,我们将收集和分析一个
丰富的基于大脑的测量数据集,具有无与伦比的分辨率和质量,
大脑网络特性的差异,并研究这些与大量表型测量指标的关系
进入关键领域的兴趣。使用静息态fMRI和创新的fMRI激活任务作为神经
社会和感官反应的分析,我们将研究如何功能连接和大脑反应,
相关的神经回路在个体内部和个体之间共同变化,以确定非典型反应性如何
感官刺激影响神经处理的社会相关的刺激,并评估如何不同的神经
社会和感觉反应的内表型与改变的功能连接和行为相关
表型在我们先前的成像遗传学工作的基础上,我们还将研究多基因风险,
ASD相关多态性的遗传变异,影响大脑功能,连接,以及核心ASD
症状我们的总体假设是,不同的和共享的神经内表型将被确定
基于不同的大脑功能和连通性指标,
在神经和行为水平上表现出的社会和感官相似性的不同维度。我们进一步
预计更高的多基因风险将预测越来越多的异常模式的大脑活动,连接,
总体症状严重程度,而ASD相关多态性的遗传变异将选择性地
调节大脑功能和这些ASD风险基因表达的大脑回路的连通性。通过
采用(a)尖端的成像方法来检查大脑功能和连接,(B)创新的
范式与社会注意力和动机的感觉处理的相似性,(c)新的方法,
将遗传风险与神经和行为表型相结合,以及(d)复杂的数据分析策略,
合理地分层我们的ASD样本,这项研究将进一步我们的神经机制的理解
ASD的潜在异质性,并最终为更个性化和有效的干预提供信息。
项目成果
期刊论文数量(1)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
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Mirella Dapretto其他文献
Mirella Dapretto的其他文献
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{{ truncateString('Mirella Dapretto', 18)}}的其他基金
1/24 Healthy Brain and Child Development National Consortium
1/24 健康大脑和儿童发展国家联盟
- 批准号:
10661784 - 财政年份:2021
- 资助金额:
$ 72.6万 - 项目类别:
Parsing ASD Heterogeneity: Neuroendophenotypes of Social Attention and Sensory Responsivity
解析 ASD 异质性:社会注意力和感觉反应的神经内表型
- 批准号:
10192837 - 财政年份:2018
- 资助金额:
$ 72.6万 - 项目类别:
Parsing ASD Heterogeneity: Neuroendophenotypes of Social Attention and Sensory Responsivity
解析 ASD 异质性:社会注意力和感觉反应的神经内表型
- 批准号:
9750309 - 财政年份:2018
- 资助金额:
$ 72.6万 - 项目类别:
Doctoral Training in Brain and Behavioral Development during Adolescence
青春期大脑和行为发展的博士培训
- 批准号:
10409573 - 财政年份:2018
- 资助金额:
$ 72.6万 - 项目类别:
Doctoral Training in Brain and Behavioral Development during Adolescence
青春期大脑和行为发展的博士培训
- 批准号:
10176170 - 财政年份:2018
- 资助金额:
$ 72.6万 - 项目类别:
Neuroimaging signatures of autism: Linking brain function to genes and behavior
自闭症的神经影像特征:将大脑功能与基因和行为联系起来
- 批准号:
8426262 - 财政年份:2012
- 资助金额:
$ 72.6万 - 项目类别:
Parsing ASD Heterogeneity: Neuroendophenotypes of Social Attention and Sensory Responsivity
解析 ASD 异质性:社会注意力和感觉反应的神经内表型
- 批准号:
10228040 - 财政年份:2007
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$ 72.6万 - 项目类别:
NEUROIMAGING LANGUAGE IN THE NORMALLY DEVELOPING BRAIN
正常发育的大脑中的神经成像语言
- 批准号:
7182838 - 财政年份:2005
- 资助金额:
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LANGUAGE, AUTISM & THE BRAIN: INSIGHTS FROM NEUROIMAGING
语言、自闭症
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6978921 - 财政年份:2004
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$ 72.6万 - 项目类别:
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