Literature DB >> 18446053

Membrane transducing activity of recombinant Hoxc8 protein and its possible application as a gene delivery vector.

Eun Shin Kim1, Myengmo Kang, Hyoung Woo Park, Myoung Hee Kim.   

Abstract

In order to examine whether the Hoxc8 protein can deliver nucleic acid into mammalian cells, we designed several Hoxc8-derived recombinant proteins to be synthesized as glutathione S-transferase (GST) fused forms in E. coli (GST-Hoxc8(1-242), containing a full length of Hoxc8; GST-Hoxc8(152-242), possessing a deletion of the acidic N-terminus of Hoxc8; GST-Hoxc8(149-208), which contained the homeodomain only). After labeling these proteins with Oregon 488, we examined their membrane transduction ability under the fluorescence microscope and verified that all three proteins showed similar transduction efficiency. The ability of the proteins to form in vitro protein-DNA complexes was analyzed on agarose gel; both GST-Hoxc8(1-242) and GST-Hoxc8(149-208) formed complexes. In contrast, the GST-Hoxc8(152-242) protein did not form a complex. The GST-Hoxc8(149-208) protein formed a complex with DNA at a mass ratio of 1ú1 (DNAúprotein), and GST-Hoxc8(1-242) formed a complex at a mass ratio of 1ú5. When the DNA (pDsRed1-C1) and protein complexes were added to culture media containing mammalian cells, the cells uptook the complexes, which was indicated by red fluorescence expression under the fluorescent microscope. These results indicate that recombinant Hoxc8 derivatives that harbor a homeodomain are able to traverse the mammalian cellular membrane. DNA that is bound to the recombinant derivatives can be carried across the membrane as well. This process could be applied in the development of a useful delivery vector for gene therapy in the future.

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Year:  2008        PMID: 18446053      PMCID: PMC2679305          DOI: 10.3858/emm.2008.40.2.151

Source DB:  PubMed          Journal:  Exp Mol Med        ISSN: 1226-3613            Impact factor:   8.718


  39 in total

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2.  Studies on the internalization mechanism of cationic cell-penetrating peptides.

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Review 3.  Cell penetrating peptides in drug delivery.

Authors:  Eric L Snyder; Steven F Dowdy
Journal:  Pharm Res       Date:  2004-03       Impact factor: 4.200

4.  Mouse naked cuticle 2 (mNkd2) as a direct transcriptional target of Hoxc8 in vivo.

Authors:  Haiyan Lei; Aster H Juan; Moo-Sang Kim; Frank H Ruddle
Journal:  J Exp Zool A Ecol Genet Physiol       Date:  2007-01-01

Review 5.  A non-covalent peptide-based strategy for protein and peptide nucleic acid transduction.

Authors:  Edwige Gros; Sebastien Deshayes; May C Morris; Gudrun Aldrian-Herrada; Julien Depollier; Frederic Heitz; Gilles Divita
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6.  Enhanced transduction of Cu,Zn-superoxide dismutase with HIV-1 Tat protein transduction domains at both termini.

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Journal:  Mol Cells       Date:  2005-04-30       Impact factor: 5.034

7.  Cationic oligopeptide-mediated delivery of dsRNA for post-transcriptional gene silencing in plant cells.

Authors:  Narayanan Unnamalai; Bong Gu Kang; Woo Sung Lee
Journal:  FEBS Lett       Date:  2004-05-21       Impact factor: 4.124

8.  Homeosis in the mouse induced by a null mutation in the Hox-3.1 gene.

Authors:  H Le Mouellic; Y Lallemand; P Brûlet
Journal:  Cell       Date:  1992-04-17       Impact factor: 41.582

Review 9.  Antitumor protein therapy; application of the protein transduction domain to the development of a protein drug for cancer treatment.

Authors:  Hiroshi Harada; Shinae Kizaka-Kondoh; Masahiro Hiraoka
Journal:  Breast Cancer       Date:  2006       Impact factor: 4.239

10.  Differential intracellular distribution of DNA complexed with polyethylenimine (PEI) and PEI-polyarginine PTD influences exogenous gene expression within live COS-7 cells.

Authors:  Stephen R Doyle; Chee Kai Chan
Journal:  Genet Vaccines Ther       Date:  2007-11-26
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