Literature DB >> 19002165

Mutational derivatives of PhiC31 integrase with increased efficiency and specificity.

Annahita Keravala1, Solomon Lee, Bhaskar Thyagarajan, Eric C Olivares, Vanessa E Gabrovsky, Lauren E Woodard, Michele P Calos.   

Abstract

phiC31 integrase is a sequence-specific phage recombinase that can recombine two short DNA sequences called attB and attP. The enzyme can also promote genomic integration of plasmids carrying attB into native mammalian sequences having partial identity to attP. To increase the efficiency of integration, we mutated the phiC31 integrase gene and screened the mutants in human cells in an assay for higher recombination frequency between attB and attP. We report in this article the isolation of a mutant, P2 that has twice the chromosomal integration frequency of wild-type phiC31 integrase, at both a preintegrated chromosomal attP site and at endogenous pseudo attP sequences in cultured human cells. In mouse liver, P2-mediated integration provided therapeutic long-term levels of human factor IX that were double those generated by wild-type phiC31 integrase. We also describe an additional mutant, P3 that combines the mutations of P2 with further changes and possesses an elevated specificity for integration at a chromosomally placed attP site in human cells. Forty-four percent of colonies carrying integration events mediated by P3 have integration at the placed attP site. These mutant integrases are useful for gene therapy and genome modification, and they demonstrate the feasibility of engineering phiC31 integrase toward more desirable properties.

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Year:  2008        PMID: 19002165      PMCID: PMC2834998          DOI: 10.1038/mt.2008.241

Source DB:  PubMed          Journal:  Mol Ther        ISSN: 1525-0016            Impact factor:   11.454


  46 in total

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6.  Site-specific genomic integration produces therapeutic Factor IX levels in mice.

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Authors:  S Kuhstoss; R N Rao
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8.  Nucleofection of muscle-derived stem cells and myoblasts with phiC31 integrase: stable expression of a full-length-dystrophin fusion gene by human myoblasts.

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  35 in total

1.  Long-term expression of human coagulation factor VIII in a tolerant mouse model using the φC31 integrase system.

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2.  Kinetics and longevity of ΦC31 integrase in mouse liver and cultured cells.

Authors:  Christopher L Chavez; Annahita Keravala; Lauren E Woodard; Robert T Hillman; Timothy R Stowe; Jacqueline N Chu; Michele P Calos
Journal:  Hum Gene Ther       Date:  2010-10       Impact factor: 5.695

3.  Generation of induced pluripotent stem cells using site-specific integration with phage integrase.

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4.  Long-term phenotypic correction in factor IX knockout mice by using ΦC31 integrase-mediated gene therapy.

Authors:  A Keravala; C L Chavez; G Hu; L E Woodard; P E Monahan; M P Calos
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5.  PhiC31 integrase induces efficient site-specific recombination in the Capra hircus genome.

Authors:  Haiyan Ma; Qingwen Ma; Yao Lu; Juan Wang; Wei Hu; Zhijuan Gong; Linlin Cai; Ying Huang; Shu-Zhen Huang; Fanyi Zeng
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7.  Impact of hydrodynamic injection and phiC31 integrase on tumor latency in a mouse model of MYC-induced hepatocellular carcinoma.

Authors:  Lauren E Woodard; Annahita Keravala; W Edward Jung; Orly L Wapinski; Qiwei Yang; Dean W Felsher; Michele P Calos
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8.  Mutational analysis of highly conserved residues in the phage phiC31 integrase reveals key amino acids necessary for the DNA recombination.

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10.  Effect of nuclear localization and hydrodynamic delivery-induced cell division on phiC31 integrase activity.

Authors:  L E Woodard; R T Hillman; A Keravala; S Lee; M P Calos
Journal:  Gene Ther       Date:  2009-10-22       Impact factor: 5.250

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