Admixture Analysis of Age at Onset in Bipolar I Affective Disorder

doi:10.1001/archpsyc.58.5.510

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Vol. 58 No. 5, May 2001

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Admixture Analysis of Age at Onset in Bipolar I Affective Disorder

Since this article does not have an abstract, we have provided the first 150 words of the full text and any section headings.

Age at onset (AAO) has frequently been a key indicator in delineating disordersubtypes leading to gene identification. Thus far, differencesin AAO have helped to separate genetic from sporadic cases incommon illnesses such as breast cancer.¹ Differences in AAO mayalso be used to identify different vulnerability genes, as inAlzheimer disease,² or different mutations in the same gene,as in Duchenne-Becker muscular dystrophy.³ More recent findingshave shown that AAO may also reflect differential expansion ofan unstable DNA region at or near the disease locus, as in myotonicdystrophy⁴ and Huntington disease.

In bipolar I affective disorder (BPAD), clinical, familial,and biological differences have been reported according to AAO.Early-onset BPAD is associated with (1) higher frequency ofaffective disorders in relatives^{5, 6, 7}; (2) higher rates ofcomorbid conditions such as psychotic symptoms during affectiveepisodes,^{7, 8, 9} lifetime panic disorder,^{9, 10} or conduct disorder,alcohol abuse, and drug . . . [Full Text of this Article]

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