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串联Alu序列转座中断人类B型肌酸激酶假基因。

Serial Alu sequence transposition interrupting a human B creatine kinase pseudogene.

作者信息

Ma T S, Ifegwu J, Watts L, Siciliano M J, Roberts R, Perryman M B

机构信息

Department of Medicine, Baylor College of Medicine, Houston, Texas 77030.

出版信息

Genomics. 1991 Jun;10(2):390-9. doi: 10.1016/0888-7543(91)90324-8.

Abstract

We have isolated, sequenced, and characterized a single-copy B creatine kinase pseudogene. The chromosomal assignment of this gene is 16p13 and a unique sequence probe from this locus detects EcoRI restriction fragment length polymorphisms of 7.8 and 5.4 kb. In 26 unrelated individuals, the frequencies for the 7.8- and 5.4-kb B creatine kinase pseudogene alleles were calculated to be 17.3 and 82.7%, respectively. The B creatine kinase pseudogene is interrupted by a 904-bp DNA insertion composed of three Alu repeat sequences in tandem flanked by an 18-bp direct repeat, derived from the pseudogene sequence. Nucleotide sequence analysis of the Alu elements suggests that the Alu sequences were incorporated into this locus in three separate integration events. Several complex clustered Alu repeat sequences without defined integration borders have been previously identified at different genomic loci. This is the first evidence that complex tandem Alu elements can integrate in an apparently serial manner in the human genome and supports the contention that Alu repeats integrate nonrandomly into the human genome.

摘要

我们已经分离、测序并鉴定了一个单拷贝的B型肌酸激酶假基因。该基因在染色体上的定位是16p13,来自该位点的一个独特序列探针可检测到7.8kb和5.4kb的EcoRI限制性片段长度多态性。在26名无关个体中,计算得出7.8kb和5.4kb的B型肌酸激酶假基因等位基因频率分别为17.3%和82.7%。B型肌酸激酶假基因被一个904bp的DNA插入片段打断,该插入片段由三个串联的Alu重复序列组成,两侧是一个18bp的直接重复序列,来源于假基因序列。对Alu元件的核苷酸序列分析表明,Alu序列是在三个独立的整合事件中整合到这个位点的。此前在不同的基因组位点已经鉴定出了几个没有明确整合边界的复杂簇状Alu重复序列。这是首次有证据表明复杂的串联Alu元件可以以明显连续的方式整合到人类基因组中,并支持了Alu重复序列非随机整合到人类基因组中的观点。

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