Literature DB >> 21780847

Differences in DNA condensation and release by lysine and arginine homopeptides govern their DNA delivery efficiencies.

Anita Mann1, Garima Thakur, Vasundhara Shukla, Anand Kamal Singh, Richa Khanduri, Rangeetha Naik, Yang Jiang, Namita Kalra, B S Dwarakanath, Ulo Langel, Munia Ganguli.   

Abstract

Designing of nanocarriers that can efficiently deliver therapeutic DNA payload and allow its smooth intracellular release for transgene expression is still a major constraint. The optimization of DNA nanocarriers requires thorough understanding of the chemical and structural characteristics of the vector-nucleic acid complexes and its correlation with the cellular entry, intracellular state and transfection efficiency. L-lysine and L-arginine based cationic peptides alone or in conjugation with other vectors are known to be putative DNA delivery agents. Here we have used L-lysine and L-arginine homopeptides of three different lengths and probed their DNA condensation and release properties by using a multitude of biophysical techniques including fluorescence spectroscopy, gel electrophoresis and atomic force microscopy. Our results clearly showed that although both lysine and arginine based homopeptides condense DNA via electrostatic interactions, they follow different pattern of DNA condensation and release in vitro. While lysine homopeptides condense DNA to form both monomolecular and multimolecular complexes and show differential release of DNA in vitro depending on the peptide length, arginine homopeptides predominantly form multimolecular complexes and show complete DNA release for all peptide lengths. The cellular uptake of the complexes and their intracellular state (as observed through flow cytometry and fluorescence microscopy) seem to be controlled by the peptide chemistry. The difference in the transfection efficiency of lysine and arginine homopeptides has been rationalized in light of these observations.

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Year:  2011        PMID: 21780847     DOI: 10.1021/mp2000814

Source DB:  PubMed          Journal:  Mol Pharm        ISSN: 1543-8384            Impact factor:   4.939


  18 in total

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4.  Amino Acid Sequence of Oligopeptide Causes Marked Difference in DNA Compaction and Transcription.

Authors:  Anatoly Zinchenko; Hiroyuki Hiramatsu; Hideaki Yamaguchi; Koji Kubo; Shizuaki Murata; Toshio Kanbe; Norio Hazemoto; Kenichi Yoshikawa; Tatsuo Akitaya
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5.  Light-mediated activation of siRNA Release in diblock copolymer assemblies for controlled gene silencing.

Authors:  Abbygail A Foster; Chad T Greco; Matthew D Green; Thomas H Epps; Millicent O Sullivan
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6.  Bioreducible polymers as a determining factor for polyplex decomplexation rate and transfection.

Authors:  Hee Sook Hwang; Han Chang Kang; You Han Bae
Journal:  Biomacromolecules       Date:  2013-01-07       Impact factor: 6.988

7.  Polyarginine molecular weight determines transfection efficiency of calcium condensed complexes.

Authors:  Nabil A Alhakamy; Cory J Berkland
Journal:  Mol Pharm       Date:  2013-04-15       Impact factor: 4.939

8.  Cellular delivery and photochemical activation of antisense agents through a nucleobase caging strategy.

Authors:  Jeane M Govan; Rajendra Uprety; Meryl Thomas; Hrvoje Lusic; Mark O Lively; Alexander Deiters
Journal:  ACS Chem Biol       Date:  2013-08-19       Impact factor: 5.100

9.  A highly efficient synthetic vector: nonhydrodynamic delivery of DNA to hepatocyte nuclei in vivo.

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Journal:  ACS Nano       Date:  2013-05-10       Impact factor: 15.881

10.  Arginine clustering on calix[4]arene macrocycles for improved cell penetration and DNA delivery.

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Journal:  Nat Commun       Date:  2013       Impact factor: 14.919

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