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精神疾病中的嵌合型脑非整倍体:低水平合子后非整倍体与精神分裂症及共病精神障碍的关联

Mosaic Brain Aneuploidy in Mental Illnesses: An Association of Low-level Post-zygotic Aneuploidy with Schizophrenia and Comorbid Psychiatric Disorders.

作者信息

Yurov Yuri B, Vorsanova Svetlana G, Demidova Irina A, Kolotii Alexei D, Soloviev Ilia V, Iourov Ivan Y

机构信息

Mental Health Research Center, Moscow, Russian Federation.

Separated Structural Unit "Clinical Research Institute of Pediatrics named after Y.E Veltishev", Pirogov Russian National Research Medical University, Moscow, Russian Federation.

出版信息

Curr Genomics. 2018 Apr;19(3):163-172. doi: 10.2174/1389202918666170717154340.

Abstract

BACKGROUND

Postzygotic chromosomal variation in neuronal cells is hypothesized to make a substantial contribution to the etiology and pathogenesis of neuropsychiatric disorders. However, the role of somatic genome instability and mosaic genome variations in common mental illnesses is a matter of conjecture.

MATERIALS AND METHODS

To estimate the pathogenic burden of somatic chromosomal mutations, we determined the frequency of mosaic aneuploidy in autopsy brain tissues of subjects with schizophrenia and other psychiatric disorders (intellectual disability comorbid with autism spectrum disorders). Recently, post-mortem brain tissues of subjects with schizophrenia, intellectual disability and unaffected controls were analyzed by Interphase Multicolor FISH (MFISH), Quantitative Fluorescent in situ Hybridization (QFISH) specially designed to register rare mosaic chromosomal mutations such as lowlevel aneuploidy (whole chromosome mosaic deletion/duplication). The low-level mosaic aneuploidy in the diseased brain demonstrated significant 2-3-fold frequency increase in schizophrenia (p=0.0028) and 4-fold increase in intellectual disability comorbid with autism (p=0.0037) compared to unaffected controls. Strong associations of low-level autosomal/sex chromosome aneuploidy (p=0.001, OR=19.0) and sex chromosome-specific mosaic aneuploidy (p=0.006, OR=9.6) with schizophrenia were revealed.

CONCLUSION

Reviewing these data and literature supports the hypothesis suggesting that an association of low-level mosaic aneuploidy with common and, probably, overlapping psychiatric disorders does exist. Accordingly, we propose a pathway for common neuropsychiatric disorders involving increased burden of rare de novo somatic chromosomal mutations manifesting as low-level mosaic aneuploidy mediating local and general brain dysfunction.

摘要

背景

神经元细胞中的合子后染色体变异被认为对神经精神疾病的病因和发病机制有重大贡献。然而,体细胞基因组不稳定性和镶嵌基因组变异在常见精神疾病中的作用仍是一个推测的问题。

材料与方法

为了估计体细胞染色体突变的致病负担,我们测定了精神分裂症和其他精神疾病(与自闭症谱系障碍共病的智力残疾)患者尸检脑组织中镶嵌非整倍体的频率。最近,通过间期多色荧光原位杂交(MFISH)、定量荧光原位杂交(QFISH)对精神分裂症、智力残疾患者及未受影响对照的死后脑组织进行分析,这些方法专门设计用于检测罕见的镶嵌染色体突变,如低水平非整倍体(全染色体镶嵌缺失/重复)。与未受影响的对照相比,患病大脑中的低水平镶嵌非整倍体在精神分裂症中频率显著增加2 - 3倍(p = 0.0028),在与自闭症共病的智力残疾中增加4倍(p = 0.0037)。揭示了低水平常染色体/性染色体非整倍体(p = 0.001,OR = 19.0)和性染色体特异性镶嵌非整倍体(p = 0.006,OR = 9.6)与精神分裂症的强关联。

结论

回顾这些数据和文献支持这样的假设,即低水平镶嵌非整倍体与常见且可能重叠的精神疾病之间确实存在关联。因此,我们提出了一条常见神经精神疾病的途径,涉及罕见的新生体细胞染色体突变负担增加,表现为低水平镶嵌非整倍体,介导局部和整体脑功能障碍。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f2e/5850504/99413bbbafe1/CG-19-163_F1.jpg

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