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与HLA - DRα基因连锁的多态性限制性内切酶位点:定位及其作为胰岛素依赖型糖尿病遗传标记的应用

Polymorphic restriction endonuclease sites linked to the HLA-DR alpha gene: localization and use as genetic markers of insulin-dependent diabetes.

作者信息

Stetler D, Grumet F C, Erlich H A

出版信息

Proc Natl Acad Sci U S A. 1985 Dec;82(23):8100-4. doi: 10.1073/pnas.82.23.8100.

Abstract

Polymorphic restriction endonuclease sites within the HLA-DR alpha gene have been defined, localized, and used as genetic markers in the analysis of susceptibility to insulin-dependent diabetes mellitus (IDDM). Hybridization of Bgl II-digested human genomic DNA with a cDNA clone for the HLA-DR alpha chain (pDR alpha-1) has revealed three allelic restriction fragment lengths: 3.8 kilobase pairs (kb), 4.2 kb, and 4.5 kb. Hybridization of EcoRV-digested human genomic DNA with the same probe has revealed two allelic polymorphic restriction fragment lengths: 9.2 kb and 13.0 kb. By analysis of double digests of genomic DNA from individuals homozygous for each of the allelic variants, the polymorphic restriction sites were found to be clustered near the 3' end of the HLA-DR alpha gene. The observed correlations of DR alpha Bgl II restriction site variants with serologically determined DR specificities suggest linkage disequilibrium between the DR alpha and DR beta loci. The 3.8-kb fragment is correlated with the DR1 type (Pc = 4.4 X 10(-4)); and the 4.2-kb fragment, with a subset (B8,DR3) of the DR3 type (Pc = 5.1 X 10(-4)) and with the DR6 type. The segregation pattern of HLA-DR alpha polymorphic Bgl II restriction fragments was analyzed in six IDDM families. The observed association of IDDM with the Bgl II 4.2-kb DR alpha restriction variant is higher than with existing serological markers and supports the utility of this approach in elucidating IDDM inheritance.

摘要

HLA - DRα基因内的多态性限制性内切酶位点已被确定、定位,并用作分析胰岛素依赖型糖尿病(IDDM)易感性的遗传标记。用HLA - DRα链的cDNA克隆(pDRα - 1)与经Bgl II消化的人类基因组DNA杂交,揭示了三种等位基因限制性片段长度:3.8千碱基对(kb)、4.2 kb和4.5 kb。用相同探针与经EcoRV消化的人类基因组DNA杂交,揭示了两种等位基因多态性限制性片段长度:9.2 kb和13.0 kb。通过对每个等位基因变体纯合个体的基因组DNA双酶切分析,发现多态性限制性位点聚集在HLA - DRα基因的3'端附近。观察到的DRα Bgl II限制性位点变体与血清学确定的DR特异性之间的相关性表明DRα和DRβ基因座之间存在连锁不平衡。3.8 kb的片段与DR1型相关(Pc = 4.4×10⁻⁴);4.2 kb的片段与DR3型的一个子集(B8,DR3)相关(Pc = 5.1×10⁻⁴)以及与DR6型相关。在六个IDDM家族中分析了HLA - DRα多态性Bgl II限制性片段的分离模式。观察到的IDDM与Bgl II 4.2 kb DRα限制性变体的关联高于与现有的血清学标记,支持了这种方法在阐明IDDM遗传方面的实用性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/210f/391450/c2bb5ad2d27c/pnas00363-0306-a.jpg

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