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Dive into the research topics where Seung-Kew Yoon is active.

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Featured researches published by Seung-Kew Yoon.


Human Gene Therapy | 2001

Cationic Liposome-Mediated Gene Delivery to the Liver and to Hepatocellular Carcinomas in Mice

Leonard Mohr; Seung-Kew Yoon; Simon J. Eastman; Quiming Chu; Ronald K. Scheule; Pier Paolo Scaglioni; Michael Geissler; Tobias Heintges; Hubert E. Blum; Jack R. Wands

The potential of cationic liposomes as nonviral vectors for in vivo gene delivery to the liver and to intrahepatic hepatocellular carcinoma (HCC) was investigated. Mice were injected via the tail vein or portal vein with a cationic lipid complexed to plasmid DNA (pDNA) encoding the chloramphenicol acetyltransferase (CAT) reporter gene at various cationic lipid:pDNA molar ratios to analyze the efficiency of gene delivery after intravenous administration. Tail vein injection resulted in high CAT expression levels in lung and spleen and low levels in the liver. Portal vein injection, by comparison, significantly enhanced hepatic reporter gene expression but also resulted in pronounced hepatic toxicity. Gene delivery to intrahepatic tumors produced by intrahepatic injection of human HCC cells was analyzed in nude mice. Tail vein injection as well as portal vein injection resulted in low levels of gene expression in intrahepatic tumors. By comparison, high levels of gene expression were achieved by direct, intratumoral injection of liposome-pDNA complexes, with only minimal expression in the surrounding normal liver. Therefore, direct liposome-pDNA complex injection appears far superior to systemic or portal intravenous administration for gene therapy of localized intrahepatic tumors, and may be a useful adjunct in the treatment of human HCCs.


Journal of Gastroenterology and Hepatology | 1997

Nucleic acid-based antiviral and gene therapy of chronic hepatitis B infection

Jack R. Wands; Michael Geissler; Jasper zu Putlitz; Hubert E. Blum; F. Von Weizsäcker; Leonhard Mohr; Seung-Kew Yoon; Margherita Melegari; Pier Paolo Scaglioni

Persistent hepatitis B virus (HBV) infection often leads to the development of chronic hepatitis, cirrhosis and hepatocellular carcinoma. There is a need to develop new antiviral approaches for the treatment of this disease. We have explored various nucleic acid‐based strategies designed to inhibit HBV replication including: the use of antisense RNA and DNA constructs, DNA‐based immunization techniques to stimulate broad‐based cellular immune responses with particular emphasis on the generation of cytotoxic lymphocyte (CTL) activity to viral structural proteins, hammerhead ribozymes to cleave HBV pregenomic RNA in vitro and dominant negative HBV core mutant proteins as inhibitors of nucleocapsid formation within cells. In order to optimize these antiviral effects, various novel expression vectors have been developed to deliver such DNA constructs to cells. For example, adenoviral vectors carrying genes that encode for dominant negative proteins have been employed to transfect hepatocytes in vitro and in vivo. In addition, plasmid vectors have been produced to promote expression of HBV structural genes following injection into muscle cells as a means to stimulate the hosts cellular and humoral immune response in the context of histocompatibility antigen (HLA) class I and II antigen presentation. These experimental approaches may have important implications for the generation of efficient antiviral effects during chronic HBV infection.


Hepatology | 2000

Gene therapy of hepatocellular carcinoma in vitro and in vivo in nude mice by adenoviral transfer of the Escherichia coli purine nucleoside phosphorylase gene

Leonhard Mohr; Srinivas Shankara; Seung-Kew Yoon; Tim U. Krohne; Michael Geissler; Bruce L. Roberts; Hubert E. Blum; Jack R. Wands


Biochemical and Biophysical Research Communications | 2000

Targeting a recombinant adenovirus vector to HCC cells using a bifunctional Fab-antibody conjugate.

Seung-Kew Yoon; Leonhard Mohr; Catherine R. O'Riordan; Amy Lachapelle; Donna Armentano; Jack R. Wands


The 59th Annual Meeting of the American Association for the Study of Liver Diseases: The Liver Meeting | 2009

FIVE YEARS OF CONTINUOUS ENTECAVIR FOR NUCLEOSIDE-NAiVE HBEAG(+) CHRONIC HEPATITIS B: RESULTS FROM STUDY ETV-901

Steven-Huy Han; Ting-Tsung Chang; You-Chen Chao; Seung-Kew Yoon; Robert G. Gish; Hugo Cheinquer; G. Kitis; Hui Zhang; Uchenna H. Iloeje


Hepatology | 2007

Four-year entecavir treatment in nucleoside-naive HBeAg(+) patients: Results from studies ETV-022 and-901

Steven Han; Ting-Tsung Chang; You-Chen Chao; Seung-Kew Yoon; Robert G. Gish; Hugo Cheinquer; Flair Jose Carrillho; Hui Zhang; Helena Brett-Smith; Robert Hindes


The Korean journal of internal medicine | 2005

Association between chronic hepatitis B virus infection and tumor necrosis factor-

J.Y. Cheong; S.W. Cho; Ki Baik Hahm; Seung-Kew Yoon; June-Hyuk Lee; Choon-Sik Park; Jong Eun Lee; Jin Hong Kim


The Korean journal of internal medicine | 2010

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Ji-Youn Yu; Chang-Wook Kim; Jin-Dong Kim; Jeong-Hyun Kwon; Jeong-Won Jang; Seung-Kew Yoon; Chang-Don Lee


The Korean journal of internal medicine | 2006

gene promoter polymorphisms

Soyeon Kim; Wonhee Her; Jong-Soon Ryu; Jing-Sang Wang; Si-Hyun Bae; Jeong-Won Jang; Chang-Wook Kim; Mi-Sook Dong; Seung-Kew Yoon


Hepatology | 2003

Autoimmune hemolytic anemia during PEG-interferon and ribavirin treatment for hepatitis C

J.Y. Cheong; Sohee Hong; Ki-Myung Lee; Seung-Kew Yoon; Dohyun Kim; Eunhee Lee; Hyunjoo Song; Byungmoo Yoo; Ki Baik Hahm; Jin Hong Kim; S.W. Cho

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Pier Paolo Scaglioni

University of Texas Southwestern Medical Center

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