Literature DB >> 11504888

Adenovirus-mediated Cre deletion of floxed sequences in primary mouse cells is an efficient alternative for studies of gene deletion.

S Prost1, S Sheahan, D Rannie, D J Harrison.   

Abstract

This study evaluates the utility of Cre-expressing adenovirus for deletion of floxed genes in primary cells using primary murine hepatocytes. Adenovirus infection was very efficient, even at very low MOI (>95% infection at a MOI of 6) and did not reduce viability. High level LacZ expression was cytotoxic to hepatocytes but Cre expression had no effect on viability. Cre-mediated recombination was completed within a timespan that permits experimentation during primary culture (>95% recombination after 24 h), independently of the number of floxed alleles per cell. Recombination did not induce p53 or produce cytological nuclear abnormalities (even in polyploid cells). Contrary to expectation, deletion of DNA ligase 1 did not alter cell cycle progression, although Cre expression hastens entry to S phase from G(1), independently of the presence of floxed sequences. We conclude that adenovirus-mediated deletion of floxed alleles in primary cells is a straightforward and highly efficient tool for conducting preliminary studies of conditional gene targeting. Primary cells have advantages of differentiation, relative purity and ease of experimentation within controlled conditions, while avoiding confounding problems encountered in vivo (i.e. target cell specificity, kinetics and level of recombination, and elicitation of inflammatory and immune responses). This system could help identify important phenotypic effects and design and interpret in vivo studies.

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Year:  2001        PMID: 11504888      PMCID: PMC55864          DOI: 10.1093/nar/29.16.e80

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


  35 in total

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2.  DNA ligase I mediates essential functions in mammalian cells.

Authors:  J H Petrini; Y Xiao; D T Weaver
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3.  Site-specific recombination mediated by an adenovirus vector expressing the Cre recombinase protein: a molecular switch for control of gene expression.

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7.  Overexpression of either liver type or pancreatic beta cell type glucokinase via recombinant adenovirus enhances glucose oxidation in isolated rat hepatocytes.

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8.  Adeno-associated virus vector mediated transduction of primary normal human breast epithelial cells.

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Authors:  S Selbert; D J Bentley; D W Melton; D Rannie; P Lourenço; C J Watson; A R Clarke
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5.  Increased FGF23 protects against detrimental cardio-renal consequences during elevated blood phosphate in CKD.

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7.  Generation of CD4CreER(T²) transgenic mice to study development of peripheral CD4-T-cells.

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8.  Adenovirus-mediated genetic removal of signaling molecules in cultured primary mouse embryonic fibroblasts.

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9.  Efficient delivery of Cre-recombinase to neurons in vivo and stable transduction of neurons using adeno-associated and lentiviral vectors.

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10.  TGFbeta induces apoptosis and EMT in primary mouse hepatocytes independently of p53, p21Cip1 or Rb status.

Authors:  Sharon Sheahan; Christopher O Bellamy; Stephen N Harland; David J Harrison; Sandrine Prost
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