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Complete MHC Haplotype Sequencing for Common Disease Gene Mapping

机译:完整的MHC单倍型测序,用于常见疾病基因定位

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摘要

The future systematic mapping of variants that confer susceptibility to common diseases requires the construction of a fully informative polymorphism map. Ideally, every base pair of the genome would be sequenced in many individuals. Here, we report 4.75 Mb of contiguous sequence for each of two common haplotypes of the major histocompatibility complex (MHC), to which susceptibility to >100 diseases has been mapped. The autoimmune disease-associated-haplotypes HLA-A3-B7-Cw7-DR15 and HLA-A1-B8-Cw7-DR3 were sequenced in their entirety through a bacterial artificial chromosome (BAC) cloning strategy using the consanguineous cell lines PGF and COX, respectively. The two sequences were annotated to encompass all described splice variants of expressed genes. We defined the complete variation content of the two haplotypes, revealing >18,000 variations between them. Average SNP densities ranged from less than one SNP per kilobase to >60. Acquisition of complete and accurate sequence data over polymorphic regions such as the MHC from large-insert cloned DNA provides a definitive resource for the construction of informative genetic maps, and avoids the limitation of chromosome regions that are refractory to PCR amplification.
机译:赋予常见疾病易感性的变体未来的系统制图需要构建一个全面的信息多态性图。理想地,基因组的每个碱基对将在许多个体中进行测序。在这里,我们报告了主要组织相容性复合体(MHC)的两个常见单倍型中每个序列的4.75 Mb连续序列,已对> 100种疾病的易感性进行了映射。使用近亲细胞系PGF和COX通过细菌人工染色体(BAC)克隆策略对自身免疫性疾病相关单倍型HLA-A3-B7-Cw7-DR15和HLA-A1-B8-Cw7-DR3进行了整体测序,分别。注释了两个序列,以涵盖所有描述的表达基因的剪接变体。我们定义了两个单元型的完整变异内容,揭示了它们之间的> 18,000个变异。平均SNP密度范围从每千个碱基不到一个SNP到> 60。从大插入克隆的DNA上获取多态性区域(例如MHC)的完整,准确的序列数据,为构建信息丰富的遗传图谱提供了确定的资源,并且避免了PCR扩增难以耐受的染色体区域的限制。

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