BRAIN PATHOPHYSIOLOGY IN ANXIETY DISORDERS
焦虑症的脑病理生理学
基本信息
- 批准号:7487904
- 负责人:
- 金额:$ 17.76万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2004
- 资助国家:美国
- 起止时间:2004-09-01 至 2009-08-31
- 项目状态:已结题
- 来源:
- 关键词:AcuteAgeAmygdaloid structureAnteriorAnxietyAnxiety DisordersAreaBehavioralBindingBrainBrain DiseasesCarbon DioxideCerebrovascular CirculationChemicalsComplementControl GroupsCore-Binding FactorDataDepressed moodDiagnosisDiagnosticDoxapramEatingEquilibriumEtiologyFrightFunctional disorderHeart RateHyperactive behaviorInfusion proceduresKnockout MiceLigandsMapsMeasuresMediatingMediator of activation proteinMentorsMentorshipMetabolicMethodologyModelingMorbidity - disease rateNeurosciencesOutcomeOutcome MeasurePanicPanic AttackPanic DisorderPathologyPatientsPatternPontine structurePositronPositron-Emission TomographyPrincipal InvestigatorProcessProsencephalonPsychopathologyPsychophysiologyRateRattusRecurrenceRegulationReportingResearchResearch TrainingRestRoleScanningSerotoninSerotonin Receptor 5-HT1ASocial PhobiaSurveysSymptomsSystemTestingTherapeuticTrainingTraining ProgramsTransgenic OrganismsVolunteer GroupWorkbasecareercomparison groupdaydesigndisabilitydisorder controlhealthy volunteerimprovedin vivointerestmouse modelneural circuitneurochemistryneuroimagingpatient orientedpre-clinicalprogramsreceptor densityrelating to nervous systemrespiratoryresponsesex
项目摘要
DESCRIPTION (provided by applicant): Panic disorder (PD) is characterized by recurrent panic attacks and severe, progressive disability. Preclinical work and neuroimaging studies suggest that pathological dysregulation of fear neurocircuitry may be fundamental to the etiology. Panic responses in PD are hypothetically mediated by overactivity in subcortical and paleocortical fear circuits and underactivity in frontal cortical processing that would otherwise serve to moderate anxiety. Efficacy of serotonergic (5-HT) therapies, reactivity to 5-HT compounds in PD and in 3reclinical anxiety models, and work in the 5-HT1A knockout mouse all point to a role for the 5-HT system in modulating pathological anxiety. The Candidate has developed a program of training and research aimed at elucidating the neural circuitry involved in the panic response in PD and defining a neurochemical deficiency that may be involved, if not etiological. Utilizing prior training in both the neuroscience of fear and the psychophysiology of PD, he plans to: 1) characterize the regional 5-HT1A binding potential in PD, an anxiety disorder control group, and a healthy volunteer group using quantitative positron emission tomography (PET) and [11C]-WAY 100635; and 2) measure change in regional cerebral blood flow (rCBF) in response to a panicogen using [150]-H20 PET in these same groups. Generalized social phobia will serve as the anxiety disorder control group due to overlapping phenomenology suggestive of commonalities in the pathological neural substrates. Defining key neurocircuitry by rCBF is considered the 1st step in a research career aimed at characterizing the chemical mediators of pathological anxiety circuits using PET. The Candidate will require intensive mentoring and didactics in PET rCBF and ligand methodologies. He has designed a 5-year program of mentorship and training by experts in the fields of neuroscience, anxiety disorders, and PET methodologies. Through such work, he seeks to contribute to the understanding of the pathophysiology of PD in order to suggest improved therapeutics for this devastating and underrecognized brain disorder.
描述(由申请人提供):惊恐障碍(PD)的特征是反复发作的惊恐发作和严重的进行性残疾。临床前工作和神经影像学研究表明,恐惧神经回路的病理失调可能是根本的病因。帕金森病的恐慌反应假设是由皮质下和古皮质恐惧回路的过度活跃和额叶皮质处理的活动不足介导的,否则会起到缓解焦虑的作用。多巴胺能(5-HT)治疗的有效性,对PD和3再临床焦虑模型中5-HT化合物的反应性,以及在5-HT 1A敲除小鼠中的作用都表明5-HT系统在调节病理性焦虑中的作用。候选人已经制定了一项培训和研究计划,旨在阐明PD恐慌反应中涉及的神经回路,并定义可能涉及的神经化学缺陷,如果不是病因的话。利用先前在恐惧神经科学和PD心理生理学方面的培训,他计划:1)使用定量正电子发射断层扫描(PET)和[11 C]-WAY 100635表征PD、焦虑症对照组和健康志愿者组的局部5-HT 1A结合潜力;和2)在这些相同的组中使用[150]-H20 PET测量响应于泛生精的局部脑血流量(rCBF)的变化。广泛性社交恐惧症将作为焦虑症的对照组,因为重叠的现象暗示了病理神经基质的共性。通过rCBF定义关键神经回路被认为是研究生涯的第一步,旨在使用PET表征病理性焦虑回路的化学介质。候选人将需要在PET rCBF和配体方法学方面的密集指导和教学。他设计了一个由神经科学、焦虑症和PET方法学领域的专家提供指导和培训的5年计划。通过这样的工作,他试图促进PD的病理生理学的理解,以便为这种破坏性和未被充分认识的大脑疾病提出改进的治疗方法。
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)
Elevated cerebrospinal fluid 5-hydroxyindoleacetic acid levels in women with comorbid depression and panic disorder.
患有抑郁症和惊恐障碍的女性脑脊液 5-羟基吲哚乙酸水平升高。
- DOI:10.1017/s1461145705006231
- 发表时间:2006
- 期刊:
- 影响因子:0
- 作者:Sullivan,GregoryM;Oquendo,MariaA;Huang,Yung-yu;Mann,JJohn
- 通讯作者:Mann,JJohn
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GREGORY M SULLIVAN其他文献
GREGORY M SULLIVAN的其他文献
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Development of TNX-1300 (Double Mutant Cocaine Esterase) for the Treatment of Life-Threatening Cocaine Intoxication
开发 TNX-1300(双突变可卡因酯酶)用于治疗危及生命的可卡因中毒
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10668212 - 财政年份:2022
- 资助金额:
$ 17.76万 - 项目类别:
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