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Linkage and association of phospholipid transfer protein activity to LASS4

机译:磷脂转移蛋白活性与LASS4的关联和关联

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摘要

Phospholipid transfer protein activity (PLTPa) is associated with insulin levels and has been implicated in atherosclerotic disease in both mice and humans. Variation at the PLTP structural locus on chromosome 20 explains some, but not all, heritable variation in PLTPa. In order to detect quantitative trait loci (QTLs) elsewhere in the genome that affect PLTPa, we performed both oligogenic and single QTL linkage analysis on four large families (n = 227 with phenotype, n = 330 with genotype, n = 462 total), ascertained for familial combined hyperlipidemia. We detected evidence of linkage between PLTPa and chromosome 19p (lod = 3.2) for a single family and chromosome 2q (lod = 2.8) for all families. Inclusion of additional marker and exome sequence data in the analysis refined the linkage signal on chromosome 19 and implicated coding variation in LASS4, a gene regulated by leptin that is involved in ceramide synthesis. Association between PLTPa and LASS4 variation was replicated in the other three families (P = 0.02), adjusting for pedigree structure. To our knowledge, this is the first example for which exome data was used in families to identify a complex QTL that is not the structural locus.
机译:磷脂转移蛋白活性(PLTPa)与胰岛素水平有关,并且与小鼠和人类的动脉粥样硬化疾病有关。第20号染色体上PLTP结构基因座的变异解释了PLTPa的一些但不是全部的遗传变异。为了检测基因组中影响PLTPa的其他地方的数量性状基因座(QTL),我们对四个大家族(表型为n = 227,基因型为n = 330,共n = 462)进行了寡聚和单QTL连锁分析,确定家族性高脂血症。我们检测到单个家庭的PLTPa和19p染色体(lod = 3.2)与所有家庭的2q染色体(lod = 2.8)之间存在连锁关系的证据。分析中包括其他标记物和外显子组序列数据,可改善19号染色体上的连锁信号,并暗示LASS4(由瘦素调节的基因,其参与神经酰胺合成)调控着编码变异。在其他三个家族(P = 0.02)中重复了PLTPa和LASS4变异之间的关联,调整了系谱结构。就我们所知,这是在家庭中使用外显子组数据来鉴定不是结构位点的复杂QTL的第一个例子。

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