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人类心脏 - 骨骼肌腺嘌呤核苷酸转位酶的基因定位及其与面肩肱型肌营养不良基因座的关系。

Genetic mapping of human heart-skeletal muscle adenine nucleotide translocator and its relationship to the facioscapulohumeral muscular dystrophy locus.

作者信息

Haraguchi Y, Chung A B, Torroni A, Stepien G, Shoffner J M, Wasmuth J J, Costigan D A, Polak M, Altherr M R, Winokur S T

机构信息

Department of Genetics and Molecular Medicine, Emory University School of Medicine, Atlanta, Georgia 30322.

出版信息

Genomics. 1993 May;16(2):479-85. doi: 10.1006/geno.1993.1214.

Abstract

The mitochondrial heart-skeletal muscle adenine nucleotide translocator (ANT1) was regionally mapped to 4q35-qter using somatic cell hybrids containing deleted chromosome 4. The regional location was further refined through family studies using ANT1 intron and promoter nucleotide polymorphisms recognized by the restriction endonucleases MboII, NdeI, and HaeIII. Two alleles were found, each at a frequency of 0.5. The ANT1 locus was found to be closely linked to D4S139, D4S171, and the dominant skeletal muscle disease locus facioscapulohumeral muscular dystrophy (FSHD). A crossover that separated D4S171 and ANT1 from D4S139 was found. Since previous studies have established the chromosome 4 map order as centromere-D4S171-D4S139-FSHD, it was concluded that ANT1 is located on the side of D4S139, that is opposite from FSHD. This conclusion was confirmed by sequencing the exons and analyzing the transcripts of ANT1 from several FSHD patients and finding no evidence of aberration.

摘要

利用含4号染色体缺失的体细胞杂种,将线粒体心脏-骨骼肌腺嘌呤核苷酸转位酶(ANT1)区域定位到4q35-qter。通过家族研究进一步细化该区域定位,这些研究使用了限制性内切酶MboII、NdeI和HaeIII识别的ANT1内含子和启动子核苷酸多态性。发现了两个等位基因,每个等位基因的频率均为0.5。发现ANT1基因座与D4S139、D4S171以及显性骨骼肌疾病基因座面肩肱型肌营养不良症(FSHD)紧密连锁。发现了一个使D4S171和ANT1与D4S139分离的交叉。由于先前的研究已确定4号染色体的图谱顺序为着丝粒-D4S171-D4S139-FSHD,因此得出结论,ANT1位于D4S139的一侧,即与FSHD相对的一侧。通过对几名FSHD患者的ANT1外显子进行测序并分析其转录本,未发现异常证据,证实了这一结论。

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