Learning, neural signaling of cortisol, and early adversity in depression
学习、皮质醇的神经信号传导和抑郁症的早期逆境
基本信息
- 批准号:8616095
- 负责人:
- 金额:$ 49.32万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2012
- 资助国家:美国
- 起止时间:2012-03-29 至 2017-02-28
- 项目状态:已结题
- 来源:
- 关键词:AccountingAction PotentialsAcuteAddressAdrenal GlandsAffectAmygdaloid structureAnimalsAwardBasic ScienceBehaviorBiological Neural NetworksBrainCognitiveCorticosteroid ReceptorsCorticotropinDataDepressed moodDepressive disorderDevelopmentDiseaseEmotionalEnvironmentEquilibriumFamilyFeedbackFemaleFunctional Magnetic Resonance ImagingFunctional disorderFutureGoalsHippocampus (Brain)HormonesHumanHydrocortisoneHypothalamic structureImpairmentIndividualInterventionKnowledgeLearningLifeLigandsLiteratureMeasurementMeasuresMediator of activation proteinMemoryMental DepressionNational Institute of Mental HealthNeurocognitivePeripheralPharmaceutical PreparationsPituitary GlandPlacebosPlasmaPrefrontal CortexProcessPublic HealthRecording of previous eventsRecoveryRegulationResearchRestRodentRoleSalineSignal TransductionStimulusStressStructureTestingTranslatingTreatment EfficacyWomanWorkanimal databaseclinical practicecostdepressive symptomsdesignearly experiencehormone regulationhuman datahydrocortisone receptorhypothalamic-pituitary-adrenal axisinnovationinterestintravenous administrationmalemeetingsmemory encodingmenneural circuitneurophysiologynovelpsychologicrelating to nervous systemresponsestemstressor
项目摘要
DESCRIPTION (provided by applicant): The "stress hormone" cortisol has been studied in depression for decades. However, relatively little is known about the role of cortisol in psychological features of depression. Basic research shows that cortisol modulates brain processes that are highly relevant to depression (especially the neural substrates of negative biases in learning and memory formation). However, very few studies have directly examined the effects of cortisol on neural circuitry of learning in depressed humans. In addition, basic research shows that the effects of cortisol on the neural substrates of learning differ for males and females. The toll of depression is especially high in women, who are roughly twice as likely as men to suffer from depression. Thus, the primary goal of this project is to investigate the effects of cortisol on the neural circuitry of learning in depressed women. A secondary goal is to investigate whether early life adversity moderates cortisol's effects on neural circuitry of learning. Animal data suggests that early life adversity causes life-long biases toward learning in threatening conditions associated with elevated cortisol. In addition, new data from humans suggests that alterations in cortisol traditionally ascribed to depression may stem in part from early adversity rather than depression per se. Thus, this study will examine effects of cortisol on neural circuitry of learning in depressed and healthy women with and without history of early life adversity. The study will use pharmacological manipulation of cortisol levels (compared to placebo) during measurement of brain activity at rest and during memory encoding of emotional and neutral stimuli. The study will also measure whether cortisol exacerbates (or instills) the negative biases in emotional memory often seen in depression. In doing so, the study will examine the role of cortisol in neural networks associated with emotional learning that are often implicated in depression. Medications that target cortisol receptors in the brain may be beneficial in the treatment of depression. However, this knowledge has yet to inform clinical practice, and mechanisms of action of these medications are not well understood. This project is significant because it provides the prerequisite knowledge (and develops a paradigm) that can be used in the development of more effective targeted intervention strategies. The project is innovative because it brings the vast literature of cortisol's effects on learning to research on depression. "Learning" broadly refers to acquisition of relevant knowledge and the capacity to adaptively alter one's behavior to meet demands of the environment. At the core of depression is difficulty adapting to and engaging with one's environmental context, especially in the face of stressors. Recovery from depression (whether treated medically or behaviorally) requires neural changes supporting adaptation to one's environment. Thus, the project translates information from animal to human research suggesting that recovery from depression entails amelioration of stress-related alterations in neural processes underlying learning.
描述(由申请人提供):几十年来,人们一直在研究“压力激素”皮质醇在抑郁症中的作用。然而,关于皮质醇在抑郁症的心理特征中的作用知之甚少。基础研究表明,皮质醇调节与抑郁症高度相关的大脑过程(特别是学习和记忆形成中负偏差的神经基质)。然而,很少有研究直接研究皮质醇对抑郁症患者学习神经回路的影响。此外,基础研究表明,皮质醇对学习的神经基质的影响对于男性和女性是不同的。抑郁症的死亡率在女性中尤其高,她们患抑郁症的可能性大约是男性的两倍。因此,这个项目的主要目标是调查皮质醇对抑郁症女性学习神经回路的影响。第二个目标是调查早期生活逆境是否会调节皮质醇对学习神经回路的影响。动物数据表明,在与皮质醇升高相关的威胁性条件下,早期生活逆境会导致终身学习偏见。此外,来自人类的新数据表明,传统上归因于抑郁症的皮质醇变化可能部分源于早期的逆境,而不是抑郁症本身。因此,本研究将探讨皮质醇对抑郁症和健康女性的学习神经回路的影响,有和没有早期生活逆境的历史。本研究将在静息时和情绪和中性刺激的记忆编码期间测量大脑活动时使用皮质醇水平的药理学操作(与安慰剂相比)。这项研究还将测量皮质醇是否会加剧(或灌输)抑郁症中常见的情绪记忆中的负面偏见。在此过程中,该研究将研究皮质醇在与情绪学习相关的神经网络中的作用,这些神经网络通常与抑郁症有关。针对大脑中皮质醇受体的药物可能对治疗抑郁症有益。然而,这些知识尚未告知临床实践,并且这些药物的作用机制尚未得到很好的理解。该项目意义重大,因为它提供了可用于制定更有效的有针对性的干预战略的先决知识(并开发了一种范例)。该项目是创新的,因为它带来了大量的文献皮质醇对学习的影响,以研究抑郁症。“学习”广义上是指获得相关知识和适应性地改变自己的行为以满足环境需求的能力。抑郁症的核心是难以适应和参与一个人的环境背景,特别是在面对压力时。从抑郁症中恢复(无论是药物治疗还是行为治疗)都需要神经变化来支持对环境的适应。因此,该项目将动物研究的信息转化为人类研究,表明从抑郁症中恢复需要改善与学习相关的神经过程中与压力相关的改变。
项目成果
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{{ truncateString('HEATHER C ABERCROMBIE', 18)}}的其他基金
Learning, neural signaling of cortisol, and early adversity in depression
学习、皮质醇的神经信号传导和抑郁症的早期逆境
- 批准号:
8450688 - 财政年份:2012
- 资助金额:
$ 49.32万 - 项目类别:
Learning, neural signaling of cortisol, and early adversity in depression
学习、皮质醇的神经信号传导和抑郁症的早期逆境
- 批准号:
8246161 - 财政年份:2012
- 资助金额:
$ 49.32万 - 项目类别:
Learning, neural signaling of cortisol, and early adversity in depression
学习、皮质醇的神经信号传导和抑郁症的早期逆境
- 批准号:
8825533 - 财政年份:2012
- 资助金额:
$ 49.32万 - 项目类别:
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