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分离出一种与囊性纤维化处于连锁不平衡状态的新DNA标记物,位于J3.11(D7S8)和IRP之间。

Isolation of a new DNA marker in linkage disequilibrium with cystic fibrosis, situated between J3.11 (D7S8) and IRP.

作者信息

Estivill X, McLean C, Nunes V, Casals T, Gallano P, Scambler P, Williamson R

机构信息

Molecular Genetics Unit, Fundació d'Investigació Santa Creu i Sant Pau, Barcelona, Spain.

出版信息

Am J Hum Genet. 1989 May;44(5):704-10.

Abstract

A cosmid library of recombinants containing nonmethylated CpG sites for rare-cutter restriction enzymes was used previously to isolate the gene IRP and four polymorphic DNA markers (pPT-3, pXV-2c, pCS.7, and pKM.19) which are close to and in linkage disequilibrium with the cystic fibrosis (CF) mutation. We have analyzed several new clones from the same library and have isolated a further cosmid, cNX.6d, which maps approximately 160 kb from CS.7, in the J3.11 direction. A DNA fragment (pMP6d-9) (D7S399) derived from cosmid cNX.6d detects a frequent polymorphism with MspI. Strong linkage disequilibrium between CF and MP6d-9 is found in European populations. Recombinations in two families suggest that CF is between the MspI polymorphic site recognized by pMP6d-9 and the polymorphism recognized by pJ3.11. The new marker is the closest, to date, to CF and will be useful for prenatal diagnosis and carrier testing.

摘要

先前使用了一个重组黏粒文库,其中包含用于稀有切割限制酶的非甲基化CpG位点,来分离基因IRP和四个多态性DNA标记(pPT-3、pXV-2c、pCS.7和pKM.19),这些标记与囊性纤维化(CF)突变紧密相邻且处于连锁不平衡状态。我们分析了来自同一文库的几个新克隆,并分离出了另一个黏粒cNX.6d,它在J3.11方向上距离CS.7约160 kb处定位。来自黏粒cNX.6d的一个DNA片段(pMP6d-9)(D7S399)可检测到MspI的常见多态性。在欧洲人群中发现CF与MP6d-9之间存在强连锁不平衡。两个家系中的重组表明CF位于pMP6d-9识别的MspI多态性位点和pJ3.11识别的多态性位点之间。这个新标记是迄今为止距离CF最近的,将有助于产前诊断和携带者检测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1059/1715644/45ce01eb231f/ajhg00115-0086-a.jpg

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