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Dive into the research topics where Young Woong Lee is active.

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Featured researches published by Young Woong Lee.


PLOS ONE | 2013

A Cancer Specific Cell-Penetrating Peptide, BR2, for the Efficient Delivery of an scFv into Cancer Cells

Ki Jung Lim; Bong Hyun Sung; Ju Ri Shin; Young Woong Lee; Da Jung Kim; Kyung Seok Yang; Sun Chang Kim

Cell-penetrating peptides (CPPs) have proven very effective as intracellular delivery vehicles for various therapeutics. However, there are some concerns about non-specific penetration and cytotoxicity of CPPs for effective cancer treatments. Herein, based on the cell-penetrating motif of an anticancer peptide, buforin IIb, we designed several CPP derivatives with cancer cell specificity. Among the derivatives, a 17-amino acid peptide (BR2) was found to have cancer-specificity without toxicity to normal cells. After specifically targeting cancer cells through interaction with gangliosides, BR2 entered cells via lipid-mediated macropinocytosis. Moreover, BR2 showed higher membrane translocation efficiency than the well-known CPP Tat (49–57). The capability of BR2 as a cancer-specific drug carrier was demonstrated by fusion of BR2 to a single-chain variable fragment (scFv) directed toward a mutated K-ras (G12V). BR2-fused scFv induced a higher degree of apoptosis than Tat-fused scFv in K-ras mutated HCT116 cells. These results suggest that the novel cell-penetrating peptide BR2 has great potential as a useful drug delivery carrier with cancer cell specificity.


Journal of Microbiology and Biotechnology | 2018

VEGF siRNA Delivery by a Cancer-Specific Cell-Penetrating Peptide

Young Woong Lee; Young Eun Hwang; Juyoung Lee; Jung-Hoon Sohn; Bong Hyun Sung; Sun Chang Kim

RNA interference provides an effective tool for developing antitumor therapies. Cell-penetrating peptides (CPPs) are delivery vectors widely used to efficiently transport small-interfering RNA (siRNA) to intracellular targets. In this study, we investigated the efficacy of the cancer-specific CPP carrier BR2 to specifically transport siRNA to cancer-target cells. Our results showed that BR2 formed a complex with anti-vascular endothelial growth factor siRNA (siVEGF) that exhibited the appropriate size and surface charge for in vivo treatment. Additionally, the BR2-VEGF siRNA complex exhibited significant serum stability and high levels of gene-silencing effects in vitro. Moreover, the transfection efficiency of the complex into a cancer cell line was higher than that observed in non-cancer cell lines, resulting in downregulated intracellular VEGF levels in HeLa cells and comprehensively improved antitumor efficacy in the absence of significant toxicity. These results indicated that BR2 has significant potential for the safe, efficient, and specific delivery of siRNA for diverse applications.


Archive | 2011

NOVEL USE OF ANTIMICROBIAL PEPTIDES IN REGENERATION OF SKIN CELLS

Sun Chang Kim; Da-Jung Kim; Su-A Jang; Bong Hyun Sung; Ki-Jung Lim; Ju-Ri Shin; Young Woong Lee


Amino Acids | 2014

Efficacy of the designer antimicrobial peptide SHAP1 in wound healing and wound infection.

Da Jung Kim; Young Woong Lee; Myung Keun Park; Ju Ri Shin; Ki Jung Lim; Ju Hyun Cho; Sun Chang Kim


Amino Acids | 2014

Erratum to: Efficacy of the designer antimicrobial peptide SHAP1 in wound healing and wound infection

Da Jung Kim; Young Woong Lee; Myung Keun Park; Ju Ri Shin; Ki Jung Lim; Ju Hyun Cho; Sun Chang Kim


Archive | 2010

NOVEL ANTICANCER AGENTS COMPRISING PEPTIDES WITH CANCER-SPECIFIC TOXICITY

Sun Chang Kim; Su A Jang; Da Jung Kim; Bong Hyun Sung; Ki Jeong Lim; Ju Ri Shin; Young Woong Lee


Archive | 2010

Multimeric antimicrobial peptide complex which is displayed on cell surface

Sun Chang Kim; Ju Ri Shin; Ki Jung Lim; Da Jung Kim; Young Woong Lee; Su A Jang; Bong Hyun Sung


Archive | 2010

Antimicrobial peptide multiblock copolymer to be expressed on surface of cells

Sun Chang Kim; Ju Ri Shin; Ki Jung Lim; Da Jung Kim; Young Woong Lee; Su A Jang; Bong Hyun Sung


Archive | 2010

Antimikrobielles peptidmultiblockcopolymer zur expression auf der oberfläche von zellen

Sun Chang Kim; Ju Ri Shin; Ki Jung Lim; Da Jung Kim; Young Woong Lee; Su A Jang; Bong Hyun Sung


Archive | 2010

Nouveaux agents anticancéreux comprenant des peptides ayant une toxicité spécifique du cancer

Sun Chang Kim; Su A Jang; Da Jung Kim; Bong Hyun Sung; Ki Jeong Lim; Ju Ri Shin; Young Woong Lee

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Bong Hyun Sung

Korea Research Institute of Bioscience and Biotechnology

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Ju Hyun Cho

Gyeongsang National University

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