Literature DB >> 2041741

Modulation of gene activity by consecutive gene targeting of one creatine kinase M allele in mouse embryonic stem cells.

J van Deursen1, R Lovell-Badge, F Oerlemans, J Schepens, B Wieringa.   

Abstract

The cytosolic creatine kinases (CK's; EC 2.7.3.2) BB, BM and MM are dimeric isoenzymes which have an important role in energy metabolism and display characteristic tissue- and stage-specific patterns of expression in mammals. To study the functional role of the distribution of the CK isoenzymes we have focussed on the modulation of expression of the genes encoding the individual B and M subunits, starting at the muscle creatine kinase (CKM) gene which is transcriptionally inactive during early embryogenesis. Using repeated rounds of gene targeting in mouse embryonic stem (ES) cells, two types of mutant cell lines were obtained. First, we generated a cell line in which insertion of a neomycin resistance (neor) gene had disrupted one of the CKM alleles. Subsequently, from this cell line, following introduction of an insertion type vector designed for replacement of the muscle specific CKM-enhancer by the constitutively acting polyoma virus enhancer PyF441, several independent doubly targeted clones were isolated which all had insertions in the previously neo-disrupted CKM allele. In some of these ES clones, the targeted enhancer replacement resulted in gene correction and functional activation of the silent CKM gene. Dimerisation between the ectopically expressed CKM subunits and CKB subunits which are normally present at high levels in ES cells, led to the formation of the BM isoform of CK in these clones.

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Year:  1991        PMID: 2041741      PMCID: PMC328181          DOI: 10.1093/nar/19.10.2637

Source DB:  PubMed          Journal:  Nucleic Acids Res        ISSN: 0305-1048            Impact factor:   16.971


  43 in total

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Authors:  S Thompson; A R Clarke; A M Pow; M L Hooper; D W Melton
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Authors:  E Robertson; A Bradley; M Kuehn; M Evans
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10.  The expression of creatine kinase isozymes in human cultured cells.

Authors:  S Povey; M Inwood; A Tanyar; M Bobrow
Journal:  Ann Hum Genet       Date:  1979-07       Impact factor: 1.670

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Review 5.  Approaching the multifaceted nature of energy metabolism: inactivation of the cytosolic creatine kinases via homologous recombination in mouse embryonic stem cells.

Authors:  J van Deursen; B Wieringa
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6.  Creatine kinase (CK) in skeletal muscle energy metabolism: a study of mouse mutants with graded reduction in muscle CK expression.

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7.  The centrosomal, putative tumor suppressor protein TACC2 is dispensable for normal development, and deficiency does not lead to cancer.

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Review 8.  Mouse genetics in the 21st century: using gene targeting to create a cornucopia of mouse mutants possessing precise genetic modifications.

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9.  Increased response to cholesterol feeding in apolipoprotein C1-deficient mice.

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10.  Targeting of the creatine kinase M gene in embryonic stem cells using isogenic and nonisogenic vectors.

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  10 in total

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