De novo CNVs in bipolar affective disorder and schizophrenia

被引:51
|
作者
Georgieva, Lyudmila [1 ]
Rees, Elliott [1 ]
Moran, Jennifer L. [2 ]
Chambert, Kimberly D. [2 ]
Milanova, Vihra [3 ]
Craddock, Nicholas [1 ]
Purcell, Shaun [4 ,5 ]
Sklar, Pamela [4 ,5 ]
McCarroll, Steven [2 ]
Holmans, Peter [1 ]
O'Donovan, Michael C. [1 ]
Owen, Michael J. [1 ]
Kirov, George [1 ]
机构
[1] Cardiff Univ, MRC, Ctr Neuropsychiat Genet & Genom, Inst Psychol Med & Clin Neurosci, Cardiff CF24 4HQ, S Glam, Wales
[2] Broad Inst MIT & Harvard, Stanley Ctr Psychiat Res, Cambridge, MA USA
[3] Med Univ, Dept Psychiat, Sofia, Bulgaria
[4] Mt Sinai Sch Med, Dept Psychiat, Div Psychiat Genom, New York, NY USA
[5] Massachusetts Gen Hosp, Psychiat & Neurodev Genet Unit, Boston, MA 02114 USA
基金
英国惠康基金; 英国医学研究理事会;
关键词
COPY NUMBER VARIANTS; ASSOCIATION; DUPLICATIONS; DELETIONS; 16P11.2; RISK;
D O I
10.1093/hmg/ddu379
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
An increased rate of de novo copy number variants (CNVs) has been found in schizophrenia (SZ), autism and developmental delay. An increased rate has also been reported in bipolar affective disorder (BD). Here, in a larger BD sample, we aimed to replicate these findings and compare de novo CNVs between SZ and BD. We used Illumina microarrays to genotype 368 BD probands, 76 SZ probands and all their parents. Copy number variants were called by PennCNV and filtered for frequency (<1%) and size (>10 kb). Putative de novo CNVs were validated with the z-score algorithm, manual inspection of log R ratios (LRR) and qPCR probes. We found 15 de novo CNVs in BD (4.1% rate) and 6 in SZ (7.9% rate). Combining results with previous studies and using a cut-off of > 100 kb, the rate of de novo CNVs in BD was intermediate between controls and SZ: 1.5% in controls, 2.2% in BD and 4.3% in SZ. Only the differences between SZ and BD and SZ and controls were significant. The median size of de novo CNVs in BD (448 kb) was also intermediate between SZ (613 kb) and controls (338 kb), but only the comparison between SZ and controls was significant. Only one de novo CNV in BD was in a confirmed SZ locus (16p11.2). Sporadic or early onset cases were not more likely to have de novo CNVs. We conclude that de novo CNVs play a smaller role in BD compared with SZ. Patients with a positive family history can also harbour de novo mutations.
引用
收藏
页码:6677 / 6683
页数:7
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