Association of the occurrence of single-nucleotide genomic variants in the genes of brain morphogenesis with a predisposition to endogenous depression in the Russian population

M. Karagyaur, A. Primak, K. D. Bozov, D. Sheleg, M. S. Arbatskiy, S. S. Dzhauari, M. E. Illarionova, E. Semina, L. Samokhodskaya, P. Klimovich, M. D. Drach, A. Velichko, E. A. Sotskaya, V. Popov, K. Rubina, M. A. Parfenenko, Yu. V. Makus, B. D. Tsygankov, V. A. Tkachuk, E. A. Neyfeld
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Abstract

Recent research indicates that some types of mental illnesses (schizophrenia, autism, depressive disorders) may be associated with impaired functioning of a number of genes, including those involved in brain morphogenesis. To assess the possible contribution of brain morphogenesis genes in the formation of predisposition to depressive disorders in Russian population, we performed whole-exome sequencing of genomic DNA of such patients. We identified 166 missense genomic variants in 66 genes (out of 140 studied) involved in the formation of brain tissue. The prevalence of some of them was estimated by allele-specific PCR. For the first time, a significantly higher frequency of occurrence of genomic variants rs17445840‑T (CDH2 gene), rs12923655‑C (CDH3 gene), rs1227051‑G/A (CDH23 gene), and rs12500437‑G/T (DCHS2 gene) was shown in a group of patients suffering from endogenous depressive disorder, and an association of some of the identified genomic variants with gender was established. The data obtained confirm the previously stated assumption that genes of brain tissue morphogenesis may be associated with a predisposition to the development of mental and cognitive disorders. The functional significance of the identified genetic variants remains to be established. The identification of pathogenic genomic variants with the confirmation of their functional significance allows better understanding of the pathogenesis of mental disorders and opens prospects for the development of approaches to objective diagnosis of such diseases, their early prevention, and pathogenetic therapy.
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俄罗斯人脑形态发生基因中的单核苷酸基因组变异与内源性抑郁症易感性之间的关系
最近的研究表明,某些类型的精神疾病(精神分裂症、自闭症、抑郁症)可能与一些基因的功能受损有关,其中包括那些参与大脑形态发生的基因。为了评估脑形态发生基因在俄罗斯人抑郁障碍易感性形成过程中可能起到的作用,我们对此类患者的基因组 DNA 进行了全外显子组测序。我们在涉及脑组织形成的 66 个基因(共 140 个)中发现了 166 个错义基因组变异。我们通过等位基因特异性 PCR 对其中一些变异的发生率进行了估计。研究首次发现,在一组内源性抑郁症患者中,rs17445840-T(CDH2 基因)、rs12923655-C(CDH3 基因)、rs1227051-G/A(CDH23 基因)和 rs12500437-G/T(DCHS2 基因)等基因组变异的出现频率明显较高,而且其中一些已确定的基因组变异还与性别有关。所获得的数据证实了之前提出的假设,即脑组织形态发生基因可能与精神和认知障碍的发病倾向有关。已确定的基因变异的功能意义仍有待确定。致病基因组变异的鉴定及其功能意义的确认有助于更好地了解精神障碍的发病机制,并为开发客观诊断此类疾病、早期预防和病理治疗的方法开辟了前景。
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