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迈向构建双相情感障碍的内表型策略。

Toward constructing an endophenotype strategy for bipolar disorders.

作者信息

Hasler Gregor, Drevets Wayne C, Gould Todd D, Gottesman Irving I, Manji Husseini K

机构信息

Mood and Anxiety Disorders Program, National Institute of Mental Health, Bethesda, Maryland, USA.

出版信息

Biol Psychiatry. 2006 Jul 15;60(2):93-105. doi: 10.1016/j.biopsych.2005.11.006. Epub 2006 Jan 9.

Abstract

Research aimed at elucidating the underlying neurobiology and genetics of bipolar disorder, and factors associated with treatment response, have been limited by a heterogeneous clinical phenotype and lack of knowledge about its underlying diathesis. We used a survey of clinical, epidemiological, neurobiological, and genetic studies to select and evaluate candidate endophenotypes for bipolar disorder. Numerous findings regarding brain function, brain structure, and response to pharmacological challenge in bipolar patients and their relatives deserve further investigation. Candidate brain function endophenotypes include attention deficits, deficits in verbal learning and memory, cognitive deficits after tryptophan depletion, circadian rhythm instability, and dysmodulation of motivation and reward. We selected reduced anterior cingulate volume and early-onset white matter abnormalities as candidate brain structure endophenotypes. Symptom provocation endophenotypes might be based on bipolar patients' sensitivity to sleep deprivation, psychostimulants, and cholinergic drugs. Phenotypic heterogeneity is a major impediment to the elucidation of the neurobiology and genetics of bipolar disorder. We present a strategy constructed to improve the phenotypic definition of bipolar disorder by elucidating candidate endophenotypes. Studies to evaluate candidate endophenotypes with respect to specificity, heritability, temporal stability, and prevalence in unaffected relatives are encouraged.

摘要

旨在阐明双相情感障碍潜在神经生物学和遗传学以及与治疗反应相关因素的研究,一直受到临床表型异质性以及对其潜在素质缺乏了解的限制。我们通过对临床、流行病学、神经生物学和遗传学研究的调查,来选择和评估双相情感障碍的候选内表型。关于双相情感障碍患者及其亲属的脑功能、脑结构以及对药物激发反应的众多发现值得进一步研究。候选脑功能内表型包括注意力缺陷、言语学习和记忆缺陷、色氨酸耗竭后的认知缺陷、昼夜节律不稳定以及动机和奖赏调节异常。我们选择前扣带回体积减小和早发性白质异常作为候选脑结构内表型。症状激发内表型可能基于双相情感障碍患者对睡眠剥夺、精神兴奋剂和胆碱能药物的敏感性。表型异质性是阐明双相情感障碍神经生物学和遗传学的主要障碍。我们提出一种通过阐明候选内表型来改善双相情感障碍表型定义的策略。鼓励开展研究以评估候选内表型在未受影响亲属中的特异性、遗传性、时间稳定性和患病率。

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