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Rapid recruitment of macrophages in interleukin-12-mediated tumour regression SCIE SCOPUS

Title
Rapid recruitment of macrophages in interleukin-12-mediated tumour regression
Authors
Ha, SJLee, SBKim, CMShin, HSSung, YC
Date Issued
1998-09
Publisher
BLACKWELL SCIENCE LTD
Abstract
In order to study the mechanism of interleukin-12 (IL-12) antitumour activity, RH7777 rat hepatoma cells were engineered to express mouse IL-12 (mIL-12) (RH7777/mIL-12) under the tight control of doxycycline (dox). The production of the mIL-12 protein was regulated by the concentration of dox that was present in the culture medium. RH7777/mIL-12 cells appeared to have the same tumorigenic activity as did parental RH7777 cells, when subcutaneously injected into syngeneic rat (BUF/N) in the absence of dox. However, the tumorigenicity of RH7777/mIL-12, but not RH7777, cells were significantly decreased when dox was administrated to the animals. In addition, established tumours of RH7777/mIL-12 cells gradually disappeared upon the induction of mIL-12, by dox, To elucidate the kinetic profile of immune cells involved in the mIL-12-induced tumour regression, both histological and immunohistochemical analyses were performed 1, 3 and 14 days after the dox treatment on rats bearing tumours that were approximately 0.5 cm in diameter, Tumour-infiltrating macrophages began to appear at the tumour site one day after dox treatment, As lime elapsed, the number of tumour infiltrates including CD4(+), CD8(+), natural killer (NK) cells and macrophages gradually increased. In particular, CD8(+) and NK cells constituted the major population of the tumour-infiltrated cells, Furthermore, it was found that resting peritoneal macrophages (PM) from rats were chemoattracted in response to mIL-12. The effects of mIL-12 on PM chemotaxis were reproducibly observed in concentrations as low as 0.1 ng/ml. These findings suggest that IL-12 can directly recruit macrophages into tumour sites which, in turn, leads to a broad and intense immunological response against tumour.
Keywords
CELL STIMULATORY FACTOR; LYMPHOCYTE MATURATION FACTOR; IFN-GAMMA PRODUCTION; BETA T-CELLS; MURINE TUMORS; GENE-THERAPY; IMMUNOREGULATORY FUNCTIONS; MAMMALIAN-CELLS; TH1 CELLS; IL-12
URI
https://oasis.postech.ac.kr/handle/2014.oak/20660
DOI
10.1046/j.1365-2567.1998.00579.x
ISSN
0019-2805
Article Type
Article
Citation
IMMUNOLOGY, vol. 95, no. 1, page. 156 - 163, 1998-09
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