Host-mediated antitumor effect of grifolan NMF-5N, a polysaccharide obtained from Grifola frondosa
Takeyama T, Suzuki I, Ohno N, Oikawa S, Sato K, Ohsawa M, Yadomae T
Tokyo College of Pharmacy, Japan.
The antitumor mechanism of grifolan
NMF-5N, a beta-1,3-glucan obtained from mycelia of
Grifola frondosa, was examined. Grifolan
NMF-5N did not show direct cytocidal effect on
cultured tumor cells. However, intraperitoneal
injection of grifolan NMF-5N increased the
number of peritoneal exudate cells and
peritoneal adherent cells which showed cytostatic activity
towards syngeneic tumor cells. In an in
vivo assay, the administration of carrageenan, an inhibitor
of macrophage function, reduced the antitumor
activity of grifolan NMF-5N. The delayed-type
hypersensitivity reaction was augmented
in the grifolan NMF-5N-administered mice. The
administration of NMF-5N augmented the
induction of cytotoxic T cells but the antitumor activity
of grifolan NMF-5N was reduced in athymic
nu/nu mice. In addition, the treatment with anti-Thy
1,2 antibody and complement C' of spleen
cells taken from mice which showed regression of
tumor due to grifolan NMF-5N, reduced the
neutralizing effect in Winn assay. These results
suggested that grifolan NMF-5N shows antitumor
activity via host-mediated mechanisms and
both macrophages and T cells play important
roles in the mechanisms.
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