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[精神分裂症的分子病理生理学及青春期预防策略]

[Molecular pathophysiology of schizophrenia and preventive strategy in pubertal period].

作者信息

Itokawa Masanari, Arai Makoto, Ichikawa Tomoe, Miyashita Mitsuhiro, Yoshikawa Takeo, Okazaki Yuji, Miyata Toshio

机构信息

Project for Schizophrenia and Affective Disorders Research, Tokyo Metropolitan Institute of Medical Science.

出版信息

Seishin Shinkeigaku Zasshi. 2011;113(7):672-8.

Abstract

A novel frameshift mutation in glyoxalase 1 (GLO1) gene was detected in a patient with schizophrenia of a pedigree with multiple affected individuals. The patient carrying the mutation showed decreased enzymatic activity by 50%, 3.7 times high level of advanced glycation end products (AGEs) that is substrate of GLO1 and 20% of serum vitamin B6 compared to controls. Case-control study of GLO1 gene suggested that Ala allele of Glu111Ala was associated with schizophrenia. In vitro study using COS-7 cells transfected with cDNA of GLO1 yielded that enzymatic activity is lower in GLO1 with Ala111 than that of Glu111. The homozygotes of Ala111 showed 16% decreased GLO1 activities in RBC as compared with that of Glu111/Ala111 and Glu111/Glu111. Plasma AGEs levels were significantly high and serum vitamin B6 was significantly low in 45 schizophrenics than that of 61 control subjects. Supplementation of vitamin B6 to cases with the genetic defect of GLO1 before onset of psychosis is suggested to be possible strategy for prevention of schizophrenia until pubertal stage since such mutation carriers could have been exposed by high level of AGEs for a long time before disease onset.

摘要

在一个有多个患者的精神分裂症家系中,一名患者被检测出乙醛脱氢酶1(GLO1)基因存在一种新的移码突变。与对照组相比,携带该突变的患者酶活性降低了50%,作为GLO1底物的晚期糖基化终产物(AGEs)水平高出3.7倍,血清维生素B6水平降低了20%。GLO1基因的病例对照研究表明,Glu111Ala的Ala等位基因与精神分裂症有关。使用转染了GLO1 cDNA的COS-7细胞进行的体外研究发现,携带Ala111的GLO1酶活性低于携带Glu111的GLO1。与Glu111/Ala111和Glu111/Glu111相比,Ala111纯合子的红细胞中GLO1活性降低了16%。45名精神分裂症患者的血浆AGEs水平显著高于61名对照受试者,血清维生素B6水平显著低于对照受试者。对于在精神病发作前存在GLO1基因缺陷的患者,在青春期前补充维生素B6可能是预防精神分裂症的一种策略,因为此类突变携带者在疾病发作前可能长期暴露于高水平的AGEs中。

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