Liver-specific Gene Delivery Using Engineered Virus-Like Particles of Hepatitis E Virus

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作者
Eun Byul Lee
Jung-Hee Kim
Wonhee Hur
Jung Eun Choi
Sung Min Kim
Dong Jun Park
Byung-Yoon Kang
Gil Won Lee
Seung Kew Yoon
机构
[1] The Catholic University of Korea,The Catholic University Liver Research Center & WHO Collaborating Center of Viral Hepatitis, Department of Biomedicine & Health Sciences
[2] am SCIENCES,undefined
[3] C-912,undefined
[4] SK V1 GL Metrocity,undefined
[5] 128,undefined
[6] Beobwonro,undefined
[7] Songpa-gu,undefined
[8] 1014,undefined
[9] A Building Gangseo-Hangang-Xi Tower 401 Yangcheon-ro,undefined
[10] Gangseo-gu,undefined
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Scientific Reports | / 9卷
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摘要
Virus-like particles (VLPs) possess great potential for organ-specific transport of therapeutic agents due to their central cavity surrounded by viral capsid proteins and similar tropism to their original viruses. The N-terminal truncated second open reading frame (Nt-ORF2) of the hepatotropic hepatitis E virus (HEV) forms VLPs via self-assembly. In the present study, we investigated whether HEV-LPs could deliver foreign genes specifically to the liver. HEV-LPs were obtained from Nt-ORF2 expression in Huh7 cells that were transduced with recombinant baculoviruses and purified by continuous density gradient centrifugation. The purified HEV-LPs efficiently penetrated liver-derived cell lines and the liver tissues. To evaluate HEV-LPs as gene delivery tools, we encapsulated foreign plasmids in HEV-LPs with disassembly/reassembly systems. Green fluorescence was detected at higher frequency in liver-derived Huh7 cells treated with HEV-LPs bearing GFP-encoding plasmids than in control cells. Additionally, HEV-LPs bearing Bax-encoding plasmids induced apoptotic signatures in Huh7 cells. In conclusion, HEV-LPs produced in mammalian cells can encapsulate foreign genes in their central cavity and specifically transport these genes to liver-derived cells, where they are expressed. The present study could contribute to advances in liver-targeted gene therapy.
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