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转基因小鼠品系中因DNA重排导致的植入后早期胚胎致死性。

Early postimplantation embryo lethality due to DNA rearrangements in a transgenic mouse strain.

作者信息

Covarrubias L, Nishida Y, Mintz B

出版信息

Proc Natl Acad Sci U S A. 1986 Aug;83(16):6020-4. doi: 10.1073/pnas.83.16.6020.

Abstract

Insertional mutagenesis in a transgenic mouse strain (HUGH/3) was caused by integration of plasmid DNA containing the human growth hormone gene and pBR322 plasmid sequences. From this study, which includes another instance of mutagenesis, and from other reports, it is apparent that insertional mutagenesis occurs fairly frequently during DNA integration in the mouse egg and that it is not specific for the exogenous DNA employed. The mutation in HUGH/3 is recessive and results in death of embryos homozygous for the donor sequences shortly after implantation, at the egg cylinder stage on days 4-5 of gestation. Restriction mapping of the insert and of the flanking DNA regions indicates that integration must have involved a series of complex events. Approximately five copies of plasmid sequences are arrayed in tandem but are interrupted at least twice by mouse cellular sequences. In addition, the mouse flanking DNA shows extensive rearrangements, probably including a deletion of at least 10 kilobases. The rearrangements may reflect an initially unstable DNA structure followed by attainment of a more stable conformation.

摘要

在一种转基因小鼠品系(HUGH/3)中,插入诱变是由含有人生长激素基因和pBR322质粒序列的质粒DNA整合引起的。从这项研究(其中包括另一个诱变实例)以及其他报告来看,很明显在小鼠卵子的DNA整合过程中插入诱变相当频繁地发生,而且它并非所使用的外源DNA所特有的。HUGH/3中的突变是隐性的,导致纯合子胚胎在植入后不久,即妊娠第4 - 5天的卵柱期死亡。对插入片段和侧翼DNA区域进行限制性图谱分析表明,整合必定涉及一系列复杂事件。大约五个质粒序列拷贝串联排列,但至少被小鼠细胞序列中断两次。此外,小鼠侧翼DNA显示出广泛的重排,可能包括至少10千碱基的缺失。这些重排可能反映了最初不稳定的DNA结构,随后达到了更稳定的构象。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f90d/386429/d250820cf01c/pnas00320-0277-a.jpg

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