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微卫星多态性分析可利用大鼠与小鼠体细胞杂种,将大鼠11β-羟化酶基因(Cyp11b1)和大鼠醛固酮合酶基因(Cyp11b2)分别定位到第7号染色体上,并可识别不同大鼠品系之间及品系内部的差异。

Microsatellite polymorphism analysis allows the individual assignment of the rat 11 beta-hydroxylase gene (Cyp11b1) and the rat aldosterone synthase gene (Cyp11b2) to chromosome 7 using rat x mouse somatic cell hybrids and identifies differences between and within various rat strains.

作者信息

Inglis G C, Kenyon C J, Szpirer C, Klinga-Levan K, Sutcliffe R G, Connell J M

机构信息

Medical Research Council, Blood Pressure Unit, Western Infirmary, Glasgow, UK.

出版信息

J Mol Endocrinol. 1995 Jun;14(3):303-11. doi: 10.1677/jme.0.0140303.

Abstract

Mouse hepatoma x rat hepatocyte hybrids that segregate rat chromosomes were used to determine the chromosomal location of the rat genes encoding 11 beta-hydroxylase and aldosterone synthase (Cyp11b1 and Cyp11b2 respectively). By means of species-specific restriction fragments and microsatellite markers both genes were mapped to rat chromosome 7. The Cyp11b1 microsatellite marker was subsequently found to vary in length between and within rat strains. Furthermore, we compared the sequences of Cyp11b1 markers in two genetically hypertensive strains of rat with their normotensive counterparts. Previous studies have indicated that 11 beta-hydroxylase activities in Milan and Lyon hypertensive strains are different from their respective genetic controls. The Cyp11b1 microsatellite regions from Lyon hypotensive and normotensive strains of rat were similar and were both shorter by 15 bases than that of the Lyon hypertensive strain. The Cyp11b1 marker in Milan hypertensive (MHS) and normotensive (MNS) strains differ from all the Lyon strains and from each other. The MHS marker is 12 bases shorter than that of MNS rats. These differences in microsatellite length may provide useful polymorphic markers in cosegregation studies of genetic hypertension in rats.

摘要

利用分离大鼠染色体的小鼠肝癌细胞与大鼠肝细胞杂交细胞系来确定编码11β-羟化酶和醛固酮合酶(分别为Cyp11b1和Cyp11b2)的大鼠基因的染色体定位。借助物种特异性限制性片段和微卫星标记,将这两个基因都定位到了大鼠的7号染色体上。随后发现Cyp11b1微卫星标记在大鼠品系之间以及同一品系内部的长度存在差异。此外,我们比较了两种遗传性高血压大鼠品系及其正常血压对照品系中Cyp11b1标记的序列。先前的研究表明,米兰和里昂高血压品系中的11β-羟化酶活性与其各自的遗传对照品系不同。来自里昂正常血压和低血压大鼠品系的Cyp11b1微卫星区域相似,且都比里昂高血压品系的短15个碱基。米兰高血压(MHS)和正常血压(MNS)品系中的Cyp11b1标记与所有里昂品系都不同,且彼此之间也不同。MHS标记比MNS大鼠的标记短12个碱基。这些微卫星长度的差异可能为大鼠遗传性高血压的共分离研究提供有用的多态性标记。

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