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首页> 外文期刊>Molecular Psychiatry >Linkage and association studies in African- and Caucasian-American populations demonstrate that SHC3 is a novel susceptibility locus for nicotine dependence
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Linkage and association studies in African- and Caucasian-American populations demonstrate that SHC3 is a novel susceptibility locus for nicotine dependence

机译:在非裔美国人和高加索裔美国人中的关联和关联研究表明,SHC3是尼古丁依赖的新型易感基因座

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摘要

Our previous linkage study demonstrated that the 9q22–q23 chromosome region showed a 'suggestive' linkage to nicotine dependence (ND) in the Framingham Heart Study population. In this study, we provide further evidence for the linkage of this region to ND in an independent sample. Within this region, the gene encoding Src homology 2 domain-containing transforming protein C3 (SHC3) represents a plausible candidate for association with ND, assessed by smoking quantity (SQ), the Heaviness of Smoking Index (HSI) and the Fagerstr?m Test for ND (FTND). We utilized 11 single-nucleotide polymorphisms within SHC3 to examine the association with ND in 602 nuclear families of either African-American (AA) or European-American (EA) origin. Individual SNP-based analysis indicated three SNPs for AAs and one for EAs were significantly associated with at least one ND measure. Haplotype analysis revealed that the haplotypes A-C-T-A-T-A of rs12519–rs3750399–rs4877042–rs2297313–rs1547696–rs1331188, with a frequency of 27.8 and 17.6%, and C-T-A-G-T of rs3750399–rs4877042–rs2297313–rs3818668–rs1547696, at a frequency of 44.7 and 30.6% in the AA and Combined samples, respectively, were significantly inversely associated with the ND measures. In the EA sample, another haplotype with a frequency of 10.6%, A-G-T-G of rs1331188–rs1556384–rs4534195–rs1411836, showed a significant inverse association with ND measures. These associations remained significant after Bonferroni correction. We further demonstrated the SHC3 contributed 40.1–59.2% (depending on the ND measures) of the linkage signals detected on chromosome 9. As further support, we found that nicotine administered through infusion increased the Shc3 mRNA level by 60% in the rat striatum, and decreased it by 22% in the nucleus accumbens (NA). At the protein level, Shc3 was decreased by 38.0% in the NA and showed no change in the striatum. Together, these findings strongly implicate SHC3 in the etiology of ND, which represents an important biological candidate for further investigation.
机译:我们之前的关联研究表明,在Framingham心脏研究人群中,9q22–q23染色体区域显示出与尼古丁依赖性(ND)的“暗示”关联。在这项研究中,我们为独立样本中该区域与ND的联系提供了进一步的证据。在该区域内,编码Src同源2结构域的转化蛋白C3(SHC3)的基因代表了与ND相关的合理候选物,通过吸烟量(SQ),吸烟指数(HSI)和Fagerstr?m检验评估ND(FTND)。我们利用SHC3中的11个单核苷酸多态性来检查与602个非裔美国人(AA)或欧美人(EA)起源的核家族中ND的关联。单个基于SNP的分析表明,AA的三个SNP和EA的一个SNP与至少一项ND措施显着相关。单倍型分析显示,rs12519–rs3750399–rs4877042–rs2297313–rs1547696–rs1331188的单倍型ACTA,频率为27.8和17.6%,rs3750399–rs4877042–rs2297313–rs3818668–rs1547696的CTAGT的频率为44.7和30.6 AA和合并样本中的%与ND度量显着负相关。在EA样本中,另一种频率为10.6%的单倍型,即rs1331188–rs1556384–rs4534195–rs1411836的A-G-T-G与ND量度呈显着负相关。 Bonferroni校正后,这些关联仍然很重要。我们进一步证明SHC3贡献了9号染色体上检测到的连锁信号的40.1–59.2 %(取决于ND量度)。作为进一步的支持,我们发现通过输注尼古丁可使大鼠Shc3 mRNA水平提高60%。纹状体,并在伏隔核(NA)中降低了22%。在蛋白质水平上,NA中的Shc3降低了38.0%,纹状体没有变化。总之,这些发现强烈暗示了SHC3在ND的病因中,它代表了进一步研究的重要生物学候选者。

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