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Analysis of gene expression and functional characterization of XPR1: a pathogenic gene for primary familial brain calcification

机译:XPR1基因表达及功能表征分析:原族脑钙化的致病基因

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摘要

Primary familial brain calcification (PFBC) is a neuropsychiatric disorder characterized by bilateral cerebral calcification with diverse neurologic or psychiatric symptoms. Recently, XPR1 variation has accounted for PFBC as another new causative gene. However, little is known about the distribution and basic function of XPR1 and its interaction with the other three pathogenic genes for PFBC (SLC20A2, PDGFRB and PDGFB). The aim of this study was to further clarify the role of XPR1 in PFBC brain pathology. As a result, gene expression profiles showed that XPR1 mRNA was widely expressed throughout the mouse brain. Cerebellum and striatum, most commonly affected in PFBC, contained a higher level of XPR1 protein than other brain regions. Additionally, XPR1 deficiency seriously affected Pi efflux and XPR1 mutations seemed to have an effect through haploinsufficiency mechanism. The immunoprecipitation and immunohistochemical studies demonstrated that XPR1 could interact with PDGFRB and might form a complex on the cell membrane. These results suggested that XPR1 played a fundamental role in the maintenance of cellular phosphate balance in the brain. This provided us with a novel perspective on understanding the pathophysiology of PFBC. The expression networks and interaction with the known pathogenic genes could shed new light on additional candidate genes for PFBC.
机译:主要家族性脑钙化(PFBC)是一种神经精神疾病,其特征,其特征,其具有不同的神经系统或精神病症状的双侧脑钙化。最近,XPR1变异已经占PFBC作为另一种新的致病基因。然而,关于XPR1的分布和碱性功能几乎熟知及其与PFBC的其他三种致病基因的相互作用(SLC20A2,PDGFRB和PDGFB)。本研究的目的是进一步阐明XPR1在PFBC脑病理中的作用。结果,基因表达谱显示XPR1 mRNA在整个小鼠脑中广泛表达。小脑和纹状体,PFBC最常见的影响,含有比其他脑区更高水平的XPR1蛋白。此外,XPR1缺陷严重影响PI Efflux和XPR1突变似乎通过臭氧机制具有效果。免疫沉淀和免疫组织化学研究表明XPR1可以与PDGFRB相互作用,并且可以在细胞膜上形成复合物。这些结果表明,XPR1在维持大脑中的细胞磷酸盐平衡方面发挥了重要作用。这为我们提供了一种关于了解PFBC病理生理学的新颖视角。表达网络和与已知致病基因的相互作用可以在PFBC的另外的候选基因上缩小新的光。

著录项

  • 来源
    《Cell and Tissue Research》 |2017年第2期|共7页
  • 作者单位

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

    Fujian Med Univ Affiliated Hosp 1 Dept Neurol 20 Chazhong Rd Fuzhou 350005 Fujian Peoples R;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

    Primary familial brain calcification; XPR1; Gene expression profiles; Phosphate efflux; Protein interactions;

    机译:主要家族脑钙化;XPR1;基因表达谱;磷酸盐;蛋白质相互作用;

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