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Review
. 2011 Dec 16;13(1):14-20.
doi: 10.1038/nrg3116.

V体育平台登录 - Genomically humanized mice: technologies and promises

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Review

Genomically humanized mice: technologies and promises

Anny Devoy et al. Nat Rev Genet. .

"V体育2025版" Abstract

Mouse models have become an invaluable tool for understanding human health and disease owing to our ability to manipulate the mouse genome exquisitely VSports手机版. Recent progress in genomic analysis has led to an increase in the number and type of disease-causing mutations detected and has also highlighted the importance of non-coding regions. As a result, there is increasing interest in creating 'genomically' humanized mouse models, in which entire human genomic loci are transferred into the mouse genome. The technical challenges towards achieving this aim are large but are starting to be tackled with success. .

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Figures

Figure 1
Figure 1. Methods of humanised mouse synthesis
There are multiple ways of introducing the human genomic region of interest into the mouse germline. (a) Traditionally this has been via an additive process, where a YAC or BAC vector is introduced via pronuclear injection or cell fusion, resulting in random incorporation into mouse genome, while the endogenous mouse locus is unmodified. (b, c) An alternative is the specific targeting and replacement of genomic loci, either using (b) homologous recombination or (c) the SSR-based technologies RMCE and RMGR. Homologous recombination with a genomic fusion (mouse-human) BAC vector results in the endogenous mouse locus being replaced by equivalent human sequence, using the large regions of homology provided by the BAC vector for increased targeting efficiency (b). RMCE and RMGR require prior modification of the mouse genome, to introduce heterotypic SSR sites to flank the region of interest. A BAC vector containing equivalent human genomic region flanked by same SSR sites then acts as a donor for the swap of genetic material mediated by expression of recombinase (c). (d) A non-integrative approach to creating a humanised mouse is by the introduction of a HAC into ES cells via MMCT. The HAC vector is synthesised via a top-down or bottom-up approach, where the genomic region of interest is introduced by homologous recombination or SSR. The HAC is mitotically stable and maintained as an extra-chromosomal element, leaving the mouse genome unmodified.

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