Intracellular delivery of nucleic acid by cell-permeable hPP10 peptide

Yi Ding; Xueli Zhao; Jingping Geng; Xiangli Guo; Jielan Ma; Hu Wang; Changbai Liu

doi:10.1002/jcp.27826

Intracellular delivery of nucleic acid by cell-permeable hPP10 peptide

Yi Ding, Xueli Zhao, Jingping Geng, Xiangli Guo, Jielan Ma, Hu Wang, Changbai Liu

Research output: Contribution to journal › Article › peer-review

Abstract

Although gene therapy offers hope against incurable diseases, nonreplicating transduction vectors remain lacking. We have previously characterized a cell-penetrating peptide hPP10 for the delivery of various cargoes; however, whether hPP10 can mediate nucleic acid delivery is still unknown. Here, examining via different ways, we demonstrate that hPP10 stably complexes with plasmid DNA (pDNA) and safely mediates nucleic acid transfection. hPP10 can mediate GFP-, dsRed-, and luciferase-expressing plasmids into cells with nearly the same efficiency as commercial transfection reagents Turbofectin or Lipofect. Furthermore, hPP10 can mediate Cre fusion protein delivery and pDNA transfection simultaneously in the Cre/loxp system in vitro. In addition, hPP10 fused with an RNA-binding domain can mediate delivery of small interfering RNA into cells to silence the reporter gene expression. Collectively, our results suggest that hPP10 is an option for nucleic acid delivery with efficiencies similar to that of commercial reagents.

Original language	English (US)
Pages (from-to)	11670-11678
Number of pages	9
Journal	Journal of Cellular Physiology
Volume	234
Issue number	7
DOIs	https://doi.org/10.1002/jcp.27826
State	Published - Jul 2019
Externally published	Yes

Keywords

cell-penetrating peptides (CPPs)
nucleic acid
small interfering RNA (siRNA), transfection

ASJC Scopus subject areas

Physiology
Clinical Biochemistry
Cell Biology

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10.1002/jcp.27826

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title = "Intracellular delivery of nucleic acid by cell-permeable hPP10 peptide",

abstract = "Although gene therapy offers hope against incurable diseases, nonreplicating transduction vectors remain lacking. We have previously characterized a cell-penetrating peptide hPP10 for the delivery of various cargoes; however, whether hPP10 can mediate nucleic acid delivery is still unknown. Here, examining via different ways, we demonstrate that hPP10 stably complexes with plasmid DNA (pDNA) and safely mediates nucleic acid transfection. hPP10 can mediate GFP-, dsRed-, and luciferase-expressing plasmids into cells with nearly the same efficiency as commercial transfection reagents Turbofectin or Lipofect. Furthermore, hPP10 can mediate Cre fusion protein delivery and pDNA transfection simultaneously in the Cre/loxp system in vitro. In addition, hPP10 fused with an RNA-binding domain can mediate delivery of small interfering RNA into cells to silence the reporter gene expression. Collectively, our results suggest that hPP10 is an option for nucleic acid delivery with efficiencies similar to that of commercial reagents.",

keywords = "cell-penetrating peptides (CPPs), nucleic acid, small interfering RNA (siRNA), transfection",

author = "Yi Ding and Xueli Zhao and Jingping Geng and Xiangli Guo and Jielan Ma and Hu Wang and Changbai Liu",

note = "Funding Information: We are thankful for the financial support by the National Natural Sciences Foundation of China (81501330), the Science Foundation of China Three Gorges University (KJ2014B066), and the Nature Science Foundation of Hubei Province (2010CDB10705). Funding Information: National Natural Sciences Foundation of China, Grant/Award Number: 81501330; Science Foundation of China Three Gorges University, Grant/Award Number: KJ2014B066; Nature Science Foundation of Hubei Province, Grant/Award Number: 2010CDB10705 Publisher Copyright: {\textcopyright} 2018 Wiley Periodicals, Inc.",

year = "2019",

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doi = "10.1002/jcp.27826",

language = "English (US)",

volume = "234",

pages = "11670--11678",

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AU - Zhao, Xueli

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AU - Guo, Xiangli

AU - Ma, Jielan

AU - Wang, Hu

AU - Liu, Changbai

N1 - Funding Information: We are thankful for the financial support by the National Natural Sciences Foundation of China (81501330), the Science Foundation of China Three Gorges University (KJ2014B066), and the Nature Science Foundation of Hubei Province (2010CDB10705). Funding Information: National Natural Sciences Foundation of China, Grant/Award Number: 81501330; Science Foundation of China Three Gorges University, Grant/Award Number: KJ2014B066; Nature Science Foundation of Hubei Province, Grant/Award Number: 2010CDB10705 Publisher Copyright: © 2018 Wiley Periodicals, Inc.

PY - 2019/7

Y1 - 2019/7

N2 - Although gene therapy offers hope against incurable diseases, nonreplicating transduction vectors remain lacking. We have previously characterized a cell-penetrating peptide hPP10 for the delivery of various cargoes; however, whether hPP10 can mediate nucleic acid delivery is still unknown. Here, examining via different ways, we demonstrate that hPP10 stably complexes with plasmid DNA (pDNA) and safely mediates nucleic acid transfection. hPP10 can mediate GFP-, dsRed-, and luciferase-expressing plasmids into cells with nearly the same efficiency as commercial transfection reagents Turbofectin or Lipofect. Furthermore, hPP10 can mediate Cre fusion protein delivery and pDNA transfection simultaneously in the Cre/loxp system in vitro. In addition, hPP10 fused with an RNA-binding domain can mediate delivery of small interfering RNA into cells to silence the reporter gene expression. Collectively, our results suggest that hPP10 is an option for nucleic acid delivery with efficiencies similar to that of commercial reagents.

AB - Although gene therapy offers hope against incurable diseases, nonreplicating transduction vectors remain lacking. We have previously characterized a cell-penetrating peptide hPP10 for the delivery of various cargoes; however, whether hPP10 can mediate nucleic acid delivery is still unknown. Here, examining via different ways, we demonstrate that hPP10 stably complexes with plasmid DNA (pDNA) and safely mediates nucleic acid transfection. hPP10 can mediate GFP-, dsRed-, and luciferase-expressing plasmids into cells with nearly the same efficiency as commercial transfection reagents Turbofectin or Lipofect. Furthermore, hPP10 can mediate Cre fusion protein delivery and pDNA transfection simultaneously in the Cre/loxp system in vitro. In addition, hPP10 fused with an RNA-binding domain can mediate delivery of small interfering RNA into cells to silence the reporter gene expression. Collectively, our results suggest that hPP10 is an option for nucleic acid delivery with efficiencies similar to that of commercial reagents.

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Intracellular delivery of nucleic acid by cell-permeable hPP10 peptide

Abstract

Keywords

ASJC Scopus subject areas

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