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首页> 外文期刊>Annals of medicine >Unraveling the complex genetics of familial combined hyperlipidemia.
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Unraveling the complex genetics of familial combined hyperlipidemia.

机译:揭示家族性高脂血症的复杂遗传学。

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Familial combined hyperlipidemia (FCHL) constitutes a substantial risk factor for atherosclerosis since it is observed in about 20% of coronary heart disease (CHD) patients under 60 years. FCHL, characterized by elevated levels of total cholesterol (TC) and triglycerides (TGs), or both, is also one of the most common familial hyperlipidemias with a prevalence of 1%-6% in Western populations. Numerous studies have been performed to identify genes contributing to FCHL. The recent linkage and association studies and their replications are beginning to elucidate the genetic variations underlying the susceptibility to FCHL. Three chromosomal regions on 1q21-23, 11p and 16q22-24.1 have been replicated in different study samples, offering targets for gene hunting. In addition, several candidate gene studies have replicated the influence of the lipoprotein lipase (LPL) gene and apolipoprotein A1/C3/A4/A5 (APOA1/C3/A4/A5) gene cluster in FCHL. Recently, the linked region on chromosome 1q21 was successfully fine-mapped and the upstream transcription factor 1 (USF1) gene identified as the underlying gene for FCHL. This finding has now been replicated in independent FCHL samples. However, the total number of variants, the risk related to each variant and their relative contributions to the disease susceptibility are not known yet.
机译:家族性合并的高脂血症(FCHL)构成动脉粥样硬化的重要危险因素,因为在60岁以下的冠心病(CHD)患者中约有20%观察到这一现象。以总胆固醇(TC)和甘油三酸酯(TGs)或两者同时升高为特征的FCHL也是最常见的家族性高脂血症之一,在西方人群中患病率为1%-6%。已经进行了大量研究以鉴定有助于FCHL的基因。最近的联系和关联研究及其复制开始阐明对FCHL易感性的潜在遗传变异。 1q21-23、11p和16q22-24.1上的三个染色体区域已在不同的研究样品中复制,为基因狩猎提供了靶标。此外,一些候选基因研究已经复制了FCHL中脂蛋白脂肪酶(LPL)基因和载脂蛋白A1 / C3 / A4 / A5(APOA1 / C3 / A4 / A5)基因簇的影响。最近,染色体1q21上的连接区域被成功地精细映射,上游转录因子1(USF1)基因被鉴定为FCHL的基础基因。现在,这一发现已被复制到独立的FCHL样本中。但是,尚不清楚变体的总数,与每个变体有关的风险及其对疾病易感性的相对贡献。

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