Antitumoral effects of recombinant adenovirus YKL-1001, conditionally replicating in α-fetoprotein-producing human liver cancer cells

Jaesung Kim; Boyoung Lee; Jin Seok Kim; Chae Ok Yun; Joo Hang Kim; Yong J. Lee; Chul Hyun Joo; Heuiran Lee

doi:10.1016/S0304-3835(02)00017-4

Antitumoral effects of recombinant adenovirus YKL-1001, conditionally replicating in α-fetoprotein-producing human liver cancer cells

Jaesung Kim, Boyoung Lee, Jin Seok Kim, Chae Ok Yun, Joo Hang Kim, Yong J. Lee, Chul Hyun Joo, Heuiran Lee

Department of Internal Medicine

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

22 Citations (Scopus)

Abstract

Selectively replicating recombinant adenovirus has emerged as a novel strategy for the treatment of incurable human cancers. One of the major characteristics of hepatocellular carcinoma is the transcriptional reactivation of α-fetoprotein (AFP). In this study, we evaluated the liver cancer-specific oncolytic potential of E1B 55kDa-deleted recombinant adenovirus (YKL-1001), which retained other E1 genes driven by the AFP promoter. Transient transfection study using luciferase indicated the selective activation of the AFP promoter only in human liver cancer cells secreting AFP (HepG2, Hep3B). YKL-1001 induced both cytopathic effects exclusively in AFP-positive liver cancer cells and the growth inhibition of pre-established Hep3B xenografts. Finally, hematoxylin-eosin staining and the immunohistochemistry to the adenoviral hexon showed a large distributed necrotic area and this implied a wide spread of YKL-1001. Therefore, the present study demonstrated that YKL-1001 holds significant promise as an oncolytic agent for hepatocellular carcinoma.

Original language	English
Pages (from-to)	23-32
Number of pages	10
Journal	Cancer Letters
Volume	180
Issue number	1
DOIs	https://doi.org/10.1016/S0304-3835(02)00017-4
Publication status	Published - 2002 Jun 6

Bibliographical note

Funding Information:
This work was supported by a grant from the Ministry of Public Health of the Republic of Korea (HMP-99-01-0008, H.L.) and a grant from the Ministry of Commerce, Industry and Energy (#990-14-05, 1999, J.-H.K.). Brain Korea 21 Project for Medical Sciences Yonsei University also supports J.-H.K. and J.K.

All Science Journal Classification (ASJC) codes

Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/S0304-3835(02)00017-4

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title = "Antitumoral effects of recombinant adenovirus YKL-1001, conditionally replicating in α-fetoprotein-producing human liver cancer cells",

abstract = "Selectively replicating recombinant adenovirus has emerged as a novel strategy for the treatment of incurable human cancers. One of the major characteristics of hepatocellular carcinoma is the transcriptional reactivation of α-fetoprotein (AFP). In this study, we evaluated the liver cancer-specific oncolytic potential of E1B 55kDa-deleted recombinant adenovirus (YKL-1001), which retained other E1 genes driven by the AFP promoter. Transient transfection study using luciferase indicated the selective activation of the AFP promoter only in human liver cancer cells secreting AFP (HepG2, Hep3B). YKL-1001 induced both cytopathic effects exclusively in AFP-positive liver cancer cells and the growth inhibition of pre-established Hep3B xenografts. Finally, hematoxylin-eosin staining and the immunohistochemistry to the adenoviral hexon showed a large distributed necrotic area and this implied a wide spread of YKL-1001. Therefore, the present study demonstrated that YKL-1001 holds significant promise as an oncolytic agent for hepatocellular carcinoma.",

author = "Jaesung Kim and Boyoung Lee and Kim, {Jin Seok} and Yun, {Chae Ok} and Kim, {Joo Hang} and Lee, {Yong J.} and Joo, {Chul Hyun} and Heuiran Lee",

note = "Funding Information: This work was supported by a grant from the Ministry of Public Health of the Republic of Korea (HMP-99-01-0008, H.L.) and a grant from the Ministry of Commerce, Industry and Energy (#990-14-05, 1999, J.-H.K.). Brain Korea 21 Project for Medical Sciences Yonsei University also supports J.-H.K. and J.K.",

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AU - Kim, Joo Hang

AU - Lee, Yong J.

AU - Joo, Chul Hyun

AU - Lee, Heuiran

N1 - Funding Information: This work was supported by a grant from the Ministry of Public Health of the Republic of Korea (HMP-99-01-0008, H.L.) and a grant from the Ministry of Commerce, Industry and Energy (#990-14-05, 1999, J.-H.K.). Brain Korea 21 Project for Medical Sciences Yonsei University also supports J.-H.K. and J.K.

PY - 2002/6/6

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N2 - Selectively replicating recombinant adenovirus has emerged as a novel strategy for the treatment of incurable human cancers. One of the major characteristics of hepatocellular carcinoma is the transcriptional reactivation of α-fetoprotein (AFP). In this study, we evaluated the liver cancer-specific oncolytic potential of E1B 55kDa-deleted recombinant adenovirus (YKL-1001), which retained other E1 genes driven by the AFP promoter. Transient transfection study using luciferase indicated the selective activation of the AFP promoter only in human liver cancer cells secreting AFP (HepG2, Hep3B). YKL-1001 induced both cytopathic effects exclusively in AFP-positive liver cancer cells and the growth inhibition of pre-established Hep3B xenografts. Finally, hematoxylin-eosin staining and the immunohistochemistry to the adenoviral hexon showed a large distributed necrotic area and this implied a wide spread of YKL-1001. Therefore, the present study demonstrated that YKL-1001 holds significant promise as an oncolytic agent for hepatocellular carcinoma.

AB - Selectively replicating recombinant adenovirus has emerged as a novel strategy for the treatment of incurable human cancers. One of the major characteristics of hepatocellular carcinoma is the transcriptional reactivation of α-fetoprotein (AFP). In this study, we evaluated the liver cancer-specific oncolytic potential of E1B 55kDa-deleted recombinant adenovirus (YKL-1001), which retained other E1 genes driven by the AFP promoter. Transient transfection study using luciferase indicated the selective activation of the AFP promoter only in human liver cancer cells secreting AFP (HepG2, Hep3B). YKL-1001 induced both cytopathic effects exclusively in AFP-positive liver cancer cells and the growth inhibition of pre-established Hep3B xenografts. Finally, hematoxylin-eosin staining and the immunohistochemistry to the adenoviral hexon showed a large distributed necrotic area and this implied a wide spread of YKL-1001. Therefore, the present study demonstrated that YKL-1001 holds significant promise as an oncolytic agent for hepatocellular carcinoma.

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Antitumoral effects of recombinant adenovirus YKL-1001, conditionally replicating in α-fetoprotein-producing human liver cancer cells

Abstract

Bibliographical note

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UN SDGs

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