特应性与染色体区域12q13 - 24的连锁及关联研究。
Studies on linkage and association of atopy with the chromosomal region 12q13-24.
作者信息
Heinzmann A, Grotherr P, Jerkic S P, Lichtenberg A, Braun S, Kruse S, Forster J, Kuehr J, Deichmann K A
机构信息
University Children's Hospital, University of Freiburg, Mathildenstrasse 1, Freiburg, Germany.
出版信息
Clin Exp Allergy. 2000 Nov;30(11):1555-61. doi: 10.1046/j.1365-2222.2000.00954.x.
BACKGROUND
Several studies have shown linkage of bronchial asthma, allergic rhinitis and total serum IgE concentration to the chromosomal region 12q13-24 in ethnical diverse populations. This region harbours a number of candidate genes for asthma and atopy, including stem cell factor (SCF), leukotriene A4 hydrolase (LTA4H), thyroid receptor 2 (TR2), and signal transducer and activator of transcription 6 (STAT6). However, the same region was shown as well to be linked to other diseases with inflammatory character. So far no variants in any of these genes have been published which would allow association studies and confirm the pathogenicity of any of these genes.
OBJECTIVE
We wanted to test for linkage of the chromosomal region 12q13-24 with the atopic phenotype without regard to clinical manifestations. Furthermore we screened for common nucleotide polymorphisms in candidate genes to enable association studies.
METHODS
We employed sib-pair linkage analysis and transmission disequilibrium testing with regard to four highly polymorphic microsatellite markers in 12q13-24 in atopic nuclear families. In addition, we looked for polymorphisms in the genes coding for SCF, LTA4H, TR2 and STAT6 performing SSCP-analysis and direct genomic sequencing.
RESULTS
We found no evidence for linkage of the genomic region 12q13-24 to elevated total serum IgE levels, specific sensitization to common inhalant allergens or atopy. Furthermore we identified three nucleotide polymorphisms including one common variant in the gene coding for SCF. No association of this polymorphism and any of the atopic phenotypes was seen.
CONCLUSION
We conclude from our data that genes in the chromosomal region 12q13-24 and in particular SCF are unlikely to exert a major effect on the induction of the atopic phenotype in our Caucasian population. However, we did not focus on the asthmatic and thereby inflammatory aspect of atopy which might explain these results in contradiction to previous studies.
背景
多项研究表明,在不同种族人群中,支气管哮喘、过敏性鼻炎和血清总IgE浓度与染色体区域12q13 - 24存在连锁关系。该区域包含许多哮喘和特应性疾病的候选基因,包括干细胞因子(SCF)、白三烯A4水解酶(LTA4H)、甲状腺受体2(TR2)以及信号转导和转录激活因子6(STAT6)。然而,该区域也显示与其他具有炎症特征的疾病存在连锁关系。到目前为止,尚未发表这些基因中的任何变异,从而无法进行关联研究并确认这些基因中任何一个的致病性。
目的
我们希望测试染色体区域12q13 - 24与特应性表型的连锁关系,而不考虑临床表现。此外,我们筛选候选基因中的常见核苷酸多态性,以进行关联研究。
方法
我们在特应性核心家庭中,针对12q13 - 24区域的四个高度多态性微卫星标记,采用同胞对连锁分析和传递不平衡检验。此外,我们通过单链构象多态性分析(SSCP)和直接基因组测序,寻找编码SCF、LTA4H、TR2和STAT6的基因中的多态性。
结果
我们没有发现基因组区域12q13 - 24与血清总IgE水平升高、对常见吸入性过敏原的特异性致敏或特应性之间存在连锁关系的证据。此外,我们鉴定出三个核苷酸多态性,其中包括编码SCF的基因中的一个常见变异。未发现该多态性与任何特应性表型之间存在关联。
结论
根据我们的数据,我们得出结论,染色体区域12q13 - 24中的基因,特别是SCF,不太可能对我们白种人群中特应性表型的诱导产生主要影响。然而,我们没有关注特应性疾病的哮喘及炎症方面,这可能解释了这些结果与先前研究相矛盾的原因。
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