Induction of manganese superoxide dismutase by an immunopotentiator as a mechanism of inhibiting of malignant progression of murine tumor cells

H Habelhah

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Journal article

Induction of manganese superoxide dismutase by an immunopotentiator as a mechanism of inhibiting of malignant progression of murine tumor cells

H Habelhah

[Hokkaido igaku zasshi] The Hokkaido journal of medical science, Vol.73(5), pp.519-529

09/1998

PMID: 9846281

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Abstract

A weakly tumorigenic cell clone (QR-32) derived from a murine fibrosarcoma (BMT-11) grew lethally in 6 out of 10 syngeneic C57BL/6 mice after co-implantation with gelatin sponge. All six cell lines (QRsP) established from the arising tumors from QR-32 had enhanced tumorigenicity and/or pulmonary metastatic ability in vivo, indicating that those QRsP cell lines acquired progressed phenotypes as compared with those of QR-32 cells. In contrast, the frequency of tumor progression was suppressed to 50% (3/6) in the cell lines (QRsP/PSK) established from those arising in the mice treated with an immunopotentiating protein-bound polysaccharide, PSK. The enhanced metastatic ability was accompanied by enhanced expressions of a tumor-associated transcription factor, E1AF and by increased production of matrix metalloproteinase (MMP) in five lines of QRsP and two lines of QRsP/PSK. It was found that administration of PSK augmented the production of an antioxidative enzyme, manganese superoxide dismutase (Mn-SOD), in the tumor tissues co-implanted with gelatin sponge. PSK administration also brought about up-regulation of interferon-gamma (IFN-gamma)-expression and down-regulation of transforming growth factor-beta (TGF-beta)-expression in the tumor tissues, which were examined by RT-PCR on day 7, 14 and 21 after the co-implantation. Other inflammatory cytokines such as interleukin-1 alpha (IL-1 alpha) and tumor necrosis factor-alpha (TNF-alpha) were expressed equally both in PSK-treated and untreated tumor tissues. In vitro experiments proved that although IFN-gamma did not increase the production of Mn-SOD by itself, concomitant treatment with both IFN-gamma and TNF-alpha enhanced the Mn-SOD-production in QR-32 cells greatly. On the contrary, TGF-beta treatment lowered the Mn-SOD level in QR-32 cells. PSK-treatment did not induce Mn-SOD in cultured QR-32 cells directly. These results indicated that PSK inhibits the malignant progression of QR-32 cells promoted by co-implantation with gelatin sponge, most possibly through elevating the Mn-SOD level in QR-32 cells via modulation of the production of inflammatory cytokines, that is, increasing IFN-gamma and decreasing TGF-beta at the site of tumor growth.

Adjuvants, Immunologic - pharmacology

Superoxide Dismutase - biosynthesis

Cytokines - metabolism

Mice, Inbred C57BL

Fibrosarcoma - therapy

Metalloendopeptidases - metabolism

Fibrosarcoma - metabolism

Disease Progression

Transcription Factors - metabolism

Neoplasm Metastasis

Proteoglycans - therapeutic use

Animals

Fibrosarcoma - pathology

Proteoglycans - pharmacology

Adenovirus E1A Proteins - metabolism

Gelatin

Enzyme Induction - drug effects

Female

Mice

Tumor Cells, Cultured

Adjuvants, Immunologic - therapeutic use

Details

Title: Subtitle: Induction of manganese superoxide dismutase by an immunopotentiator as a mechanism of inhibiting of malignant progression of murine tumor cells
Creators: H Habelhah - Laboratory of Pathology, Hokkaido University School of Medicine, Sapporo, Japan
Resource Type: Journal article
Publication Details: [Hokkaido igaku zasshi] The Hokkaido journal of medical science, Vol.73(5), pp.519-529
PMID: 9846281
NLM abbreviation: Hokkaido Igaku Zasshi
ISSN: 0367-6102
Publisher: Japan
Language: Japanese
Date published: 09/1998
Academic Unit: Pathology
Record Identifier: 9984047607102771

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