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首页> 外文期刊>Genes and immunity. >Circulating MCP-1 levels shows linkage to chemokine receptor gene cluster on chromosome 3: the NHLBI family heart study follow-up examination.
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Circulating MCP-1 levels shows linkage to chemokine receptor gene cluster on chromosome 3: the NHLBI family heart study follow-up examination.

机译:循环中的MCP-1水平显示与3号染色体上趋化因子受体基因簇的连锁关系:NHLBI家族心脏研究随访检查。

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Atherogenesis is a chronic inflammatory process. Critical in the inflammation process is monocyte chemoattractant protein-1 (MCP-1). To locate genomic regions that affect circulating MCP-1 levels, a genome-wide linkage scan was conducted in a sample of whites and blacks. Phenotype and genetic marker data were available for 2501 white and 513 black participants in the National Heart Lung Blood Institute Family Heart Study follow-up examination. Heritability for MCP-1 was 0.37 in whites and 0.47 in blacks after adjusting for the effects of sex, age, age-sex interaction, smoking status, lifetime smoking exposure (pack-years) and field center. Significant linkage was observed for MCP-1 in a combined black and white sample on chromosome 3 (logarithm of the odds ratio (LOD)=3.5 at 78 cM, P=0.0001) and suggestive linkage was observed in whites on chromosome 5 (LOD=1.8 at 128 cM, P=0.002). Located under the linkage peak on chromosome 3 is the chemokine receptor gene cluster, including CCR2, the receptor for MCP-1. This study provides preliminary evidence linking genetic variation in a receptor to circulating levels of its ligand, as previously demonstrated for the low-density lipoprotein receptor. Further characterization of these chromosomal regions is needed to identify the functional mutations associated with circulating levels of MCP-1.
机译:动脉粥样硬化是慢性炎症过程。在炎症过程中至关重要的是单核细胞趋化蛋白1(MCP-1)。为了定位影响循环MCP-1水平的基因组区域,对白人和黑人样本进行了全基因组连锁扫描。在美国国家心肺血液研究所家庭心脏研究随访检查中,有2501名白人和513名黑人参与者获得了表型和遗传标记数据。调整性别,年龄,年龄-性别相互作用,吸烟状况,终生吸烟暴露(包装年)和田野中心的影响后,白人中MCP-1的遗传力为0.37,黑人为0.47。在3号染色体上的黑白组合样品中观察到了MCP-1的显着连锁(在78 cM时,优势比(LOD)的对数= 3.5,P = 0.0001),在5号染色体上的白色中观察到了暗示的连锁(LOD =在128 cM时为1.8,P = 0.002)。趋化因子受体基因簇位于染色体3的连锁峰之下,包括MCP-1的受体CCR2。这项研究提供了将受体的遗传变异与其配体的循环水平相关联的初步证据,如先前针对低密度脂蛋白受体所证明的。需要进一步表征这些染色体区域,以鉴定与MCP-1循环水平相关的功能突变。

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