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lacI转基因小鼠DNA突变随年龄的比较分析。

Comparative analysis of DNA mutations in lacI transgenic mice with age.

作者信息

Lee A T, DeSimone C, Cerami A, Bucala R

机构信息

Picower Institute for Medical Research, Manhasset, New York 11030.

出版信息

FASEB J. 1994 May;8(8):545-50. doi: 10.1096/fasebj.8.8.8181674.

DOI:10.1096/fasebj.8.8.8181674
PMID:8181674
Abstract

Transgenic mice have been developed recently that contain copies of the well-defined mutagenesis reporter gene, lacI, in an integrated bacteriophage-based shuttle vector. The lacI gene, which is present in all cells of the mouse, can be excised specifically from isolated genomic DNA and efficiently packaged into bacteriophage particles after the addition of packaging extracts. Mutations of the lacI gene are easily detected by the derepression of beta-galactosidase resulting in blue plaques in the presence of X-gal. Originally developed as a short-term in vivo mutagenesis assay to screen genotoxic agents, we have used this system to measure naturally occurring DNA mutations as a function of chronological age. There was a linear increase in the presence of phenotypic lacI mutants from birth to 24 months (r = 0.731, P < 0.001), such that 24-month-old mice have accumulated approximately fourfold more mutants than newborn pups. Molecular analysis of these spontaneously arising DNA mutations showed them to result predominantly from base substitutions (80.6-98.5%) that were equally distributed between transitions and transversions. However, lacI mutations in animals > 3 months of age demonstrated a higher percentage of mutations (12-19.4% vs. 1.2%) resulting from discriminable size changes (> 20 bp) than was observed for mice 1-2 months old. Sequence analysis of mutations resulting from a > 20 bp size change revealed them to be due to a duplication of adjacent lacI sequence. These results indicate that there is a gradual accumulation of DNA mutations with age and that the types of mutations also are influenced by the age of the animal.

摘要

最近已培育出转基因小鼠,其在基于噬菌体的整合穿梭载体中含有明确定义的诱变报告基因lacI的拷贝。lacI基因存在于小鼠的所有细胞中,在加入包装提取物后,可从分离的基因组DNA中特异性切除,并有效包装到噬菌体颗粒中。在X-gal存在的情况下,β-半乳糖苷酶的去抑制作用可轻松检测到lacI基因的突变,从而产生蓝色噬菌斑。该系统最初是作为一种短期体内诱变试验来筛选遗传毒性剂的,我们已使用此系统来测量作为时间年龄函数的自然发生的DNA突变。从出生到24个月,表型lacI突变体的数量呈线性增加(r = 0.731,P < 0.001),因此24个月大的小鼠积累的突变体比新生幼崽多约四倍。对这些自发产生的DNA突变的分子分析表明,它们主要由碱基替换(80.6 - 98.5%)引起,转换和颠换之间分布均匀。然而,与1 - 2个月大的小鼠相比,3个月以上动物中的lacI突变显示出由可辨别大小变化(> 20 bp)导致的突变百分比更高(12 - 19.4%对1.2%)。对由> 20 bp大小变化导致的突变进行序列分析发现,它们是由于相邻lacI序列的重复所致。这些结果表明,DNA突变会随着年龄逐渐积累,并且突变类型也受动物年龄的影响。

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