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Prolongation of the survival of breast cancer-bearing mice immunized with GM-CSF-secreting syngeneic/allogeneic fibroblasts transfected with a cDNA expression library from breast cancer cells

Authors
Kim, Tae S.Jung, Mi Y.Cho, DaehoCohen, Edward P.
Issue Date
Oct-2006
Publisher
ELSEVIER SCI LTD
Keywords
breast cancer; fibroblast; GM-CSF; tumor immunity; vaccine
Citation
VACCINE, v.24, no.42-43, pp 6564 - 6573
Pages
10
Journal Title
VACCINE
Volume
24
Number
42-43
Start Page
6564
End Page
6573
URI
https://scholarworks.sookmyung.ac.kr/handle/2020.sw.sookmyung/15052
DOI
10.1016/j.vaccine.2006.06.012
ISSN
0264-410X
1358-8745
Abstract
Breast cancer cells, like other types of neoplastic cells, form weakly immunogenic tumor-associated antigens. The antigenic properties of the tumor-associated antigens can be enhanced if they are expressed by highly immunogenic cells. In this study, a cancer vaccine was prepared by transfer of a cDNA expression library from SB5b breast carcinoma into mouse fibroblast cells of C3H/He mouse origin (H-2(k)), that had been previously modified to secrete GM-CSF and to express allogeneic class I-determinants (H-2(b)). The transfected syngeneic/allogeneic fibroblasts secreting GM-CSF were used as a vaccine in C3H/He mice. Robust cell-mediated immunity toward the breast cancer cells was generated in mice immunized with the cDNA-based vaccine. The immunity, mediated predominantly by CD8(+) T lymphocytes, was directed toward the breast cancer cells, but not against either of two other non-cross-reactive neoplasms of OH/He mice. The immunity was sufficient to prolong the survival of mice with established breast cancer. Among other advantages, preparation of the vaccine by cDNA-transfer into a fibroblast cell line enabled the recipient cells to be modified in advance of DNA-transfer to augment their immunogenic properties. As the transferred DNA is replicated as the transfected cells divide, the vaccine could be prepared from microgram quantities of tumor tissue. (c) 2006 Elsevier Ltd. All rights reserved.
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