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G72 primate-specific gene: a still enigmatic element in psychiatric disorders

机译:G72灵长类动物特异性基因:在精神疾病中仍是一个谜

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Numerous studies have demonstrated a link between genetic markers on chromosome 13 and schizophrenia, bipolar affective disorder, and other psychiatric phenotypes. The G72/G30 genes (transcribed in opposite directions) are located on chromosome 13q33, a region demonstrating strong evidence for linkage with various neuropsychiatric disorders. G72/G30 was identified in 2002 as a schizophrenia susceptibility locus; however, subsequent association studies did not reach consensus on single SNPs within the locus. Simultaneously, a new vision for the genetic architecture of psychiatric disorders suggested that schizophrenia was a quantitative trait, therefore ascribable to potentially hundreds of genes and subjected to the vagaries of the environment. The main protein product of G72 gene is named pLG72 or d-amino acid oxidase activator DAOA (153 amino acids) and its function is still debated. Functional analyses, also showing controversial results, indicate that pLG72 contributes to N-methyl-d-aspartate receptor modulation by affecting activity of the flavoprotein d-amino acid oxidase, the enzyme responsible for degrading the neuromodulator d-serine. In this review we, for the first time, summarize findings from molecular genetic linkage and association studies concerning G72 gene, cellular and molecular studies on pLG72, and investigations performed on G72/G30 transgenic mice. This will help elucidate the role of psychosis susceptibility genes, which will have a major impact on our understanding of disease pathophysiology and thus change classification and treatment.
机译:大量研究表明,第13号染色体上的遗传标记与精神分裂症,双相情感障碍和其他精神病学表型之间存在联系。 G72 / G30基因(转录方向相反)位于染色体13q33上,该区域显示出与各种神经精神疾病相关的有力证据。 G72 / G30在2002年被确定为精神分裂症的易感基因座;但是,随后的关联研究并未就位点内的单个SNP达成共识。同时,对精神疾病遗传结构的新视野表明,精神分裂症是一种定量性状,因此归因于潜在的数百种基因,并且易受环境变化的影响。 G72基因的主要蛋白质产物称为pLG72或d-氨基酸氧化酶激活剂DAOA(153个氨基酸),其功能仍在争论中。功能分析也显示了有争议的结果,表明pLG72通过影响黄素蛋白d-氨基酸氧化酶(负责降解神经调节剂d-丝氨酸的酶)的活性来促进N-甲基-d-天冬氨酸受体的调节。在本综述中,我们首次总结了有关G72基因的分子遗传连锁和关联研究,对pLG72的细胞和分子研究以及对G72 / G30转基因小鼠进行的研究的发现。这将有助于阐明精神病易感基因的作用,这将对我们对疾病病理生理学的理解产生重大影响,从而改变分类和治疗。

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