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69个双相情感障碍家系复制集中精神病性症状的家族聚集性。

Familial aggregation of psychotic symptoms in a replication set of 69 bipolar disorder pedigrees.

作者信息

Potash James B, Chiu Yen-Feng, MacKinnon Dean F, Miller Erin B, Simpson Sylvia G, McMahon Francis J, McInnis Melvin G, DePaulo J Raymond

机构信息

Department of Psychiatry and Behavioral Sciences, Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.

出版信息

Am J Med Genet B Neuropsychiatr Genet. 2003 Jan 1;116B(1):90-7. doi: 10.1002/ajmg.b.10761.

Abstract

We found evidence previously of familial aggregation of psychotic symptoms in 65 bipolar disorder pedigrees. This finding, together with prior evidence from clinical, family, neurobiological, and linkage studies, suggested that psychotic bipolar disorder may delineate a valid subtype. We sought to replicate this finding in 69 new bipolar disorder pedigrees. The presence of psychotic symptoms, defined as hallucinations or delusions, during an affective episode was compared in families of 46 psychotic and 23 non-psychotic bipolar I probands ascertained at Johns Hopkins for the NIMH Bipolar Disorder Genetics Initiative. There were 198 first-degree relatives with major affective disorder including 90 with bipolar I disorder. Significantly more psychotic proband families than non-psychotic proband families (76% vs. 48%) contained at least one affected relative with psychotic symptoms. Psychotic symptoms occurred in 35% of relatives of psychotic probands and in 22% of relatives of non-psychotic probands (P = 0.10). Both psychotic affective disorder generally and psychotic bipolar I disorder clustered significantly in families. These results are consistent with our prior report although the magnitude of the predictive effect of a psychotic proband is less in the replication families. Our findings provide modest support for the validity of psychotic bipolar disorder as a subtype of bipolar disorder. This clinically defined subtype may prove more homogeneous than the disorder as a whole at the level of genetic etiology and of neuropathology/pathophysiology. Families with this subtype should be used to search for susceptibility genes common to bipolar disorder and schizophrenia, and for biological markers that may be shared with schizophrenia.

摘要

我们之前在65个双相情感障碍家系中发现了精神病性症状的家族聚集性证据。这一发现,连同临床、家族、神经生物学和连锁研究的先前证据,表明精神病性双相情感障碍可能是一个有效的亚型。我们试图在69个新的双相情感障碍家系中重复这一发现。在约翰·霍普金斯大学为美国国立精神卫生研究所双相情感障碍遗传学倡议确定的46名患有精神病性症状的双相I型先证者和23名非精神病性双相I型先证者的家庭中,比较了情感发作期间幻觉或妄想定义的精神病性症状的存在情况。有198名患有重度情感障碍的一级亲属,其中90名患有双相I型障碍。患有精神病性症状的先证者家庭比非精神病性先证者家庭(76%对48%)包含至少一名患有精神病性症状的受影响亲属的比例显著更高。35%的精神病性先证者亲属和22%的非精神病性先证者亲属出现了精神病性症状(P = 0.10)。精神病性情感障碍总体以及精神病性双相I型障碍在家族中都有显著聚集。这些结果与我们之前的报告一致,尽管在重复研究的家系中,精神病性先证者的预测效应程度较小。我们的发现为精神病性双相情感障碍作为双相情感障碍的一个亚型的有效性提供了适度支持。这个临床定义的亚型在遗传病因学和神经病理学/病理生理学水平上可能比整个双相情感障碍更具同质性。患有这种亚型的家系应用于寻找双相情感障碍和精神分裂症共有的易感基因,以及可能与精神分裂症共享的生物学标志物。

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