Tumor-specific gene transfer via an adenoviral vector targeted to the pan-carcinoma antigen EpCAM

H J Haisma; H M Pinedo; A L van Rijswijk; Ida H. van der Meulen-Muileman; B A Sosnowski; W Ying; B W Tillman; D T Curiel; VW van Beusechem; W.R. Gerritsen

doi:https://doi.org/10.1038/sj.gt.3300969

Tumor-specific gene transfer via an adenoviral vector targeted to the pan-carcinoma antigen EpCAM

H J Haisma, H M Pinedo, A L van Rijswijk, Ida H. van der Meulen-Muileman, B A Sosnowski, W Ying, B W Tillman, D T Curiel, VW van Beusechem, W.R. Gerritsen

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

112 Citations (Scopus)

Abstract

The utility of adenoviral vectors for cancer therapy is limited due to their lack of specificity for tumor cells. In order to target adenovirus to tumor, the natural tropism of the adenovirus should be ablated and replaced by a tumor-specific binding domain. To this end, a neutralizing anti-fiber antibody conjugated to an anti-EpCAM antibody was created that targets the adenovirus to the EpCAM antigen present on tumor cells. The EpCAM antigen was chosen as the target because this antigen is highly expressed on a variety of adenocarcinomas of different origin such as breast, ovary, colon and lung, whereas EpCAM expression is limited in normal tissues. In these studies, the EpCAM-targeted adenovirus was shown to infect specifically cancer cell lines of different origin expressing EpCAM such as ovary, colon and head and neck. Gene transfer was blocked by excess anti-EpCAM antibody and dramatically reduced in EpCAM negative cell lines, thus showing the specificity of the EpCAM-targeted adenovirus. Importantly, infection with targeted adenovirus was independent of CAR, which is the natural receptor for adenovirus binding, since blocking of CAR with recombinant fiber knob did not affect infection with targeted adenovirus. Apart from the cancer cell lines, the efficacy of targeted viral infection was studied in freshly isolated primary human colon cancer cells. As colon cancer predominantly metastasizes to liver, and adenovirus has a high tropism for hepatocytes, we also sought to determine if the EpCAM-targeted adenovirus showed reduced infectivity of human liver cells. The bispecific antibody could successfully mediate gene transfer to primary human colon cancer cells, whereas it almost completely abolished infection of liver cells. This work thus demonstrates that EpCAM-targeted adenoviral vectors can be specifically directed to a wide variety of adenocarcinomas. This approach may prove to be useful for selective gene therapy of cancer.

Original language	English
Pages (from-to)	1469-74
Number of pages	6
Journal	Gene therapy
Volume	6
Issue number	8
DOIs	https://doi.org/10.1038/sj.gt.3300969
Publication status	Published - Aug 1999

Keywords

Adenocarcinoma/therapy
Adenoviridae/genetics
Antigens, Neoplasm/genetics
Cell Adhesion Molecules/genetics
Colonic Neoplasms/therapy
Epithelial Cell Adhesion Molecule
Gene Targeting/methods
Gene Transfer Techniques
Genetic Therapy/methods
Genetic Vectors/genetics
Humans
Integrins/metabolism
Tumor Cells, Cultured

Access to Document

https://doi.org/10.1038/sj.gt.3300969

Cite this

@article{66ad30d708ba4022971b5a574b530ced,

title = "Tumor-specific gene transfer via an adenoviral vector targeted to the pan-carcinoma antigen EpCAM",

abstract = "The utility of adenoviral vectors for cancer therapy is limited due to their lack of specificity for tumor cells. In order to target adenovirus to tumor, the natural tropism of the adenovirus should be ablated and replaced by a tumor-specific binding domain. To this end, a neutralizing anti-fiber antibody conjugated to an anti-EpCAM antibody was created that targets the adenovirus to the EpCAM antigen present on tumor cells. The EpCAM antigen was chosen as the target because this antigen is highly expressed on a variety of adenocarcinomas of different origin such as breast, ovary, colon and lung, whereas EpCAM expression is limited in normal tissues. In these studies, the EpCAM-targeted adenovirus was shown to infect specifically cancer cell lines of different origin expressing EpCAM such as ovary, colon and head and neck. Gene transfer was blocked by excess anti-EpCAM antibody and dramatically reduced in EpCAM negative cell lines, thus showing the specificity of the EpCAM-targeted adenovirus. Importantly, infection with targeted adenovirus was independent of CAR, which is the natural receptor for adenovirus binding, since blocking of CAR with recombinant fiber knob did not affect infection with targeted adenovirus. Apart from the cancer cell lines, the efficacy of targeted viral infection was studied in freshly isolated primary human colon cancer cells. As colon cancer predominantly metastasizes to liver, and adenovirus has a high tropism for hepatocytes, we also sought to determine if the EpCAM-targeted adenovirus showed reduced infectivity of human liver cells. The bispecific antibody could successfully mediate gene transfer to primary human colon cancer cells, whereas it almost completely abolished infection of liver cells. This work thus demonstrates that EpCAM-targeted adenoviral vectors can be specifically directed to a wide variety of adenocarcinomas. This approach may prove to be useful for selective gene therapy of cancer.",

keywords = "Adenocarcinoma/therapy, Adenoviridae/genetics, Antigens, Neoplasm/genetics, Cell Adhesion Molecules/genetics, Colonic Neoplasms/therapy, Epithelial Cell Adhesion Molecule, Gene Targeting/methods, Gene Transfer Techniques, Genetic Therapy/methods, Genetic Vectors/genetics, Humans, Integrins/metabolism, Tumor Cells, Cultured",

author = "Haisma, {H J} and Pinedo, {H M} and {van Rijswijk}, {A L} and {van der Meulen-Muileman}, {Ida H.} and Sosnowski, {B A} and W Ying and Tillman, {B W} and Curiel, {D T} and {van Beusechem}, VW and W.R. Gerritsen",

year = "1999",

month = aug,

doi = "https://doi.org/10.1038/sj.gt.3300969",

language = "English",

volume = "6",

pages = "1469--74",

journal = "Gene therapy",

issn = "0969-7128",

publisher = "Nature Publishing Group",

number = "8",

}

TY - JOUR

T1 - Tumor-specific gene transfer via an adenoviral vector targeted to the pan-carcinoma antigen EpCAM

AU - Haisma, H J

AU - Pinedo, H M

AU - van Rijswijk, A L

AU - van der Meulen-Muileman, Ida H.

AU - Sosnowski, B A

AU - Ying, W

AU - Tillman, B W

AU - Curiel, D T

AU - van Beusechem, VW

AU - Gerritsen, W.R.

PY - 1999/8

Y1 - 1999/8

N2 - The utility of adenoviral vectors for cancer therapy is limited due to their lack of specificity for tumor cells. In order to target adenovirus to tumor, the natural tropism of the adenovirus should be ablated and replaced by a tumor-specific binding domain. To this end, a neutralizing anti-fiber antibody conjugated to an anti-EpCAM antibody was created that targets the adenovirus to the EpCAM antigen present on tumor cells. The EpCAM antigen was chosen as the target because this antigen is highly expressed on a variety of adenocarcinomas of different origin such as breast, ovary, colon and lung, whereas EpCAM expression is limited in normal tissues. In these studies, the EpCAM-targeted adenovirus was shown to infect specifically cancer cell lines of different origin expressing EpCAM such as ovary, colon and head and neck. Gene transfer was blocked by excess anti-EpCAM antibody and dramatically reduced in EpCAM negative cell lines, thus showing the specificity of the EpCAM-targeted adenovirus. Importantly, infection with targeted adenovirus was independent of CAR, which is the natural receptor for adenovirus binding, since blocking of CAR with recombinant fiber knob did not affect infection with targeted adenovirus. Apart from the cancer cell lines, the efficacy of targeted viral infection was studied in freshly isolated primary human colon cancer cells. As colon cancer predominantly metastasizes to liver, and adenovirus has a high tropism for hepatocytes, we also sought to determine if the EpCAM-targeted adenovirus showed reduced infectivity of human liver cells. The bispecific antibody could successfully mediate gene transfer to primary human colon cancer cells, whereas it almost completely abolished infection of liver cells. This work thus demonstrates that EpCAM-targeted adenoviral vectors can be specifically directed to a wide variety of adenocarcinomas. This approach may prove to be useful for selective gene therapy of cancer.

AB - The utility of adenoviral vectors for cancer therapy is limited due to their lack of specificity for tumor cells. In order to target adenovirus to tumor, the natural tropism of the adenovirus should be ablated and replaced by a tumor-specific binding domain. To this end, a neutralizing anti-fiber antibody conjugated to an anti-EpCAM antibody was created that targets the adenovirus to the EpCAM antigen present on tumor cells. The EpCAM antigen was chosen as the target because this antigen is highly expressed on a variety of adenocarcinomas of different origin such as breast, ovary, colon and lung, whereas EpCAM expression is limited in normal tissues. In these studies, the EpCAM-targeted adenovirus was shown to infect specifically cancer cell lines of different origin expressing EpCAM such as ovary, colon and head and neck. Gene transfer was blocked by excess anti-EpCAM antibody and dramatically reduced in EpCAM negative cell lines, thus showing the specificity of the EpCAM-targeted adenovirus. Importantly, infection with targeted adenovirus was independent of CAR, which is the natural receptor for adenovirus binding, since blocking of CAR with recombinant fiber knob did not affect infection with targeted adenovirus. Apart from the cancer cell lines, the efficacy of targeted viral infection was studied in freshly isolated primary human colon cancer cells. As colon cancer predominantly metastasizes to liver, and adenovirus has a high tropism for hepatocytes, we also sought to determine if the EpCAM-targeted adenovirus showed reduced infectivity of human liver cells. The bispecific antibody could successfully mediate gene transfer to primary human colon cancer cells, whereas it almost completely abolished infection of liver cells. This work thus demonstrates that EpCAM-targeted adenoviral vectors can be specifically directed to a wide variety of adenocarcinomas. This approach may prove to be useful for selective gene therapy of cancer.

KW - Adenocarcinoma/therapy

KW - Adenoviridae/genetics

KW - Antigens, Neoplasm/genetics

KW - Cell Adhesion Molecules/genetics

KW - Colonic Neoplasms/therapy

KW - Epithelial Cell Adhesion Molecule

KW - Gene Targeting/methods

KW - Gene Transfer Techniques

KW - Genetic Therapy/methods

KW - Genetic Vectors/genetics

KW - Humans

KW - Integrins/metabolism

KW - Tumor Cells, Cultured

U2 - https://doi.org/10.1038/sj.gt.3300969

DO - https://doi.org/10.1038/sj.gt.3300969

M3 - Article

C2 - 10467371

SN - 0969-7128

VL - 6

SP - 1469

EP - 1474

JO - Gene therapy

JF - Gene therapy

IS - 8

ER -