Literature DB >> 10899153

Interdigitated deletion complexes on mouse chromosome 5 induced by irradiation of embryonic stem cells.

J C Schimenti1, B J Libby, R A Bergstrom, L A Wilson, D Naf, L M Tarantino, A Alavizadeh, A Lengeling, M Bucan.   

Abstract

Chromosome deletions have several applications in the genetic analysis of complex organisms. They can be used as reagents in region-directed mutagenesis, for mapping of simple or complex traits, or to identify biological consequences of segmental haploidy, the latter being relevant to human contiguous gene syndromes and imprinting. We have generated three deletion complexes in ES (Embryonic Stem) cells that collectively span approximately 40 cM of proximal mouse chromosome 5. The deletion complexes were produced by irradiation of F(1) hybrid ES cells containing herpes simplex virus thymidine kinase genes (tk) integrated at the Dpp6, Hdh (Huntington disease locus), or Gabrb1 loci, followed by selection for tk-deficient clones. Deletions centered at the adjacent Hdh and Dpp6 loci ranged up to approximately 20 cM or more in length and overlapped in an interdigitated fashion. However, the interval between Hdh and Gabrb1 appeared to contain a locus haploinsufficient for ES cell viability, thereby preventing deletions of either complex from overlapping. In some cases, the deletions resolved the order of markers that were previously genetically inseparable. A subset of the ES cell-bearing deletions was injected into blastocysts to generate germline chimeras and establish lines of mice segregating the deletion chromosomes. At least 11 of the 26 lines injected were capable of producing germline chimeras. In general, those that failed to undergo germline transmission bore deletions larger than the germline-competent clones, suggesting that certain regions of chromosome 5 contain haploinsufficient developmental genes, and/or that overall embryonic viability is cumulatively decreased as more genes are rendered hemizygous. Mice bearing deletions presumably spanning the semidominant hammertoe locus (Hm) had no phenotype, suggesting that the classic allele is a dominant, gain-of-function mutation. Overlapping deletion complexes generated in the fashion described in this report will be useful as multipurpose genetic tools and in systematic functional mapping of the mouse genome.

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Year:  2000        PMID: 10899153      PMCID: PMC310891          DOI: 10.1101/gr.10.7.1043

Source DB:  PubMed          Journal:  Genome Res        ISSN: 1088-9051            Impact factor:   9.043


  29 in total

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Authors:  H te Riele; E R Maandag; A Berns
Journal:  Proc Natl Acad Sci U S A       Date:  1992-06-01       Impact factor: 11.205

3.  The albino-deletion complex of the mouse: molecular mapping of deletion breakpoints that define regions necessary for development of the embryonic and extraembryonic ectoderm.

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Journal:  Genetics       Date:  1991-11       Impact factor: 4.562

4.  Germ-line intrachromosomal recombination restores fertility in transgenic MyK-103 male mice.

Authors:  T M Wilkie; R E Braun; W J Ehrman; R D Palmiter; R E Hammer
Journal:  Genes Dev       Date:  1991-01       Impact factor: 11.361

5.  Genetic mapping of the mouse gene encoding dipeptidyl aminopeptidase-like proteins.

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Journal:  Mamm Genome       Date:  1993       Impact factor: 2.957

6.  Gene targeting in embryonic stem cells.

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Journal:  Methods Enzymol       Date:  1993       Impact factor: 1.600

7.  Msx1 is close but not allelic to either Hm or Hx on mouse chromosome 5.

Authors:  B Robert; X Montagutelli; D Houzelstein; L Ferland; A Cohen; M Buckingham; J L Guénet
Journal:  Mamm Genome       Date:  1994-07       Impact factor: 2.957

8.  Analysis of the albino-locus region of the mouse: IV. Characterization of 34 deficiencies.

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9.  Congenital heart disease in mice deficient for the DiGeorge syndrome region.

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10.  Molecular genetics of the brown (b)-locus region of mouse chromosome 4. I. Origin and molecular mapping of radiation- and chemical-induced lethal brown deletions.

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  11 in total

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2.  Functional annotation of mammalian genomic DNA sequence by chemical mutagenesis: a fine-structure genetic mutation map of a 1- to 2-cM segment of mouse chromosome 7 corresponding to human chromosome 11p14-p15.

Authors:  Eugene M Rinchik; Donald A Carpenter; Dabney K Johnson
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3.  Creating a "hopeful monster": mouse forward genetic screens.

Authors:  Vanessa L Horner; Tamara Caspary
Journal:  Methods Mol Biol       Date:  2011

4.  X-ray-induced deletion complexes in embryonic stem cells on mouse chromosome 15.

Authors:  Wallace S H Chick; Sarah E Mentzer; Donald A Carpenter; Eugene M Rinchik; Dabney Johnson; Yun You
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5.  Random mutagenesis of proximal mouse chromosome 5 uncovers predominantly embryonic lethal mutations.

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Journal:  Genome Res       Date:  2005-07-15       Impact factor: 9.043

6.  Mouse H6 Homeobox 1 (Hmx1) mutations cause cranial abnormalities and reduced body mass.

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7.  Functional annotation of mouse mutations in embryonic stem cells by use of expression profiling.

Authors:  Derek J Symula; Yiwen Zhu; John C Schimenti; Edward M Rubin
Journal:  Mamm Genome       Date:  2004-01       Impact factor: 2.957

8.  Overlapping deletions spanning the proximal two-thirds of the mouse t complex.

Authors:  David E Bergstrom; Rebecca A Bergstrom; Robert J Munroe; Barbara K Lee; Victoria L Browning; Yun You; Eva M Eicher; John C Schimenti
Journal:  Mamm Genome       Date:  2003-12       Impact factor: 2.957

9.  High resolution mapping and positional cloning of ENU-induced mutations in the Rw region of mouse chromosome 5.

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10.  Slingshot: a PiggyBac based transposon system for tamoxifen-inducible 'self-inactivating' insertional mutagenesis.

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