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首页> 外文期刊>Undersea and Hyperbaric Medicine: Journal of the Undersea and Hyperbaric Medical Society >HPNS seizure risk: a role for the Golgi-associated retrograde protein complex?
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HPNS seizure risk: a role for the Golgi-associated retrograde protein complex?

机译:Golgi-associated HPNS发作风险:一个角色逆行性蛋白质复杂吗?

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摘要

Previous attempts to characterize the genetic contribution to differential risk of developing the HPNS seizure in a mouse model system are extended to additional data and an analytical mode that incorporates the set of linked resources for systems genetics in the GeneNetwork project. A quantitative trait locus (QTL) affecting HPNS seizure phenotype was mapped to a approximately 6 megabase (Mb) gene-rich region of Chr 17 based on the degree of expression covariation among genes in the region of the QTL and genes in the brains of BXD recombinant inbred mice in the same chromosomal region. Use of GeneNetwork's WebQTL analytical modules revealed that among > 220 positional candidate genes, vacuolar protein sorting gene 52 (Vps52) has highest priority. It appears that a single nearly null mutation in a distal region of Vps52 3'UTR (untranslated region) defined by a DNA probe set is associated with > 60% of the seizure risk difference between the high- and low-risk strains DBA/2 and C57BL/6, respectively. Based on the known contribution of the elements of the GARP complex--Vps52, -53 and -54--to motoneuron abnormalities, mutation-depleted Vps52 may be implicated in HPNS seizure risk variation in the mouse and, by gene homology, also with human VPS52.
机译:以前曾试图描述遗传对微分的风险的贡献HPNS发作在一个小鼠模型系统扩展到更多的数据和分析模式包含链接的集合GeneNetwork系统遗传学的资源项目。影响HPNS发作表型被映射到一个大约6 megabase (Mb)拥有的地区科17基于表达式的程度相关变异基因中QTL区域在BXD的大脑和基因重组成小鼠在相同的染色体区域。GeneNetwork WebQTL分析模块显示在> 220位置候选基因,空泡的蛋白基因排序52 (Vps52)最高优先级。零Vps52 3 'utr远地区的突变(翻译区)定义为一组DNA探针与> 60%的发作风险高和低风险品种之间的差异分别DBA / 2和C57BL / 6,。已知的元素GARP的贡献复杂——Vps52, -53年和-54年——运动神经元异常,mutation-depleted Vps52涉及HPNS发作风险的变化鼠标和基因同源性,也与人类

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