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人类肾上腺素能受体基因的遗传图谱

Genetic mapping of adrenergic receptor genes in humans.

作者信息

Hoehe M R, Otterud B, Hsieh W T, Martinez M M, Stauffer D, Holik J, Berrettini W H, Byerley W F, Gershon E S, Lalouel J M

机构信息

Max Delbrück Center for Molecular Medicine, Berlin-Buch, Germany.

出版信息

J Mol Med (Berl). 1995 Jun;73(6):299-306. doi: 10.1007/BF00231616.

DOI:10.1007/BF00231616
PMID:7583452
Abstract

We have genetically mapped the genes encoding four human adrenergic receptors (ARs) of subtypes alpha 1C, alpha 2A, alpha 2B, and beta 1, which are prototypic G protein coupled receptors that mediate the physiological effects of neurotransmitters, hormones, and drugs. We placed these genes onto the Cooperative Human Linkage Center (CHLC) and Genethon framework maps, within confidence intervals with greater than 1000:1 odds. With multipoint analysis the alpha 1C gene (locus ADRA1C) mapped to the interval between NEFL and D8S283; alpha 2-C4, the gene encoding the alpha 2C AR (locus ADRA2C), mapped to the interval between D4S126 and D4S62; and the alpha 2-C10 (alpha 2A AR)/beta 1 haplotype (loci ADRA2A/ADRB1) mapped to the interval between D10S259 and D10S187. A fifth AR gene, beta 2, yielded significant LOD scores with markers on the long arm of chromosome 5; however, this locus (ADRB2) could not be mapped to any specific interval with odds of greater than 1000:1. The two AR genes that are completely linked, alpha 2-C10 and beta 1, were oriented on their shared 225-kb genomic fragment relative to the direction of transcription, with beta 1 being 5' to alpha 2-C10. The positioning of these genes on high-density framework maps allows them to be tested as candidates in a spectrum of diseases that might involve AR dysfunction.

摘要

我们已经对编码四种人类肾上腺素能受体(ARs)亚型α1C、α2A、α2B和β1的基因进行了遗传定位,这些受体是典型的G蛋白偶联受体,介导神经递质、激素和药物的生理效应。我们将这些基因定位到合作人类连锁中心(CHLC)和吉内通框架图谱上,置信区间的优势比大于1000:1。通过多点分析,α1C基因(基因座ADRA1C)定位到NEFL和D8S283之间的区间;编码α2C AR的基因α2-C4(基因座ADRA2C)定位到D4S126和D4S62之间的区间;α2-C10(α2A AR)/β1单倍型(基因座ADRA2A/ADRB1)定位到D10S259和D10S187之间的区间。第五个AR基因β2与5号染色体长臂上的标记产生了显著的LOD分数;然而,该基因座(ADRB2)无法定位到优势比大于1000:1的任何特定区间。完全连锁的两个AR基因α2-C10和β1,在其共享的225kb基因组片段上相对于转录方向进行了定向,β1在α2-C10的5'端。这些基因在高密度框架图谱上的定位使其能够作为可能涉及AR功能障碍的一系列疾病的候选基因进行检测。

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Genetic mapping of adrenergic receptor genes in humans.人类肾上腺素能受体基因的遗传图谱
J Mol Med (Berl). 1995 Jun;73(6):299-306. doi: 10.1007/BF00231616.
2
Haplotype-based analysis of alpha 2A, 2B, and 2C adrenergic receptor genes captures information on common functional loci at each gene.基于单倍型的α2A、2B和2C肾上腺素能受体基因分析获取了每个基因常见功能位点的信息。
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Genes encoding adrenergic receptors are not clustered on the long arm of human chromosome 5.编码肾上腺素能受体的基因并非聚集在人类5号染色体的长臂上。
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Adrenergic receptor genes as candidate genes for panic disorder: a linkage study.肾上腺素能受体基因作为惊恐障碍的候选基因:一项连锁研究。
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Chromosomal organization of adrenergic receptor genes.肾上腺素能受体基因的染色体组织
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Genomics. 1993 Sep;17(3):611-7. doi: 10.1006/geno.1993.1380.

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2
Pharmacogenomics in heart failure: where are we now and how can we reach clinical application?心力衰竭中的药物基因组学:我们目前的进展如何以及如何实现临床应用?
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