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L5178Y小鼠肿瘤休眠状态的免疫调节。II. 干扰素-γ需要肿瘤坏死因子来抑制来自肿瘤休眠小鼠的腹膜细胞培养物中的肿瘤细胞生长。

Immune regulation of the L5178Y murine tumor-dormant state. II. Interferon-gamma requires tumor necrosis factor to restrain tumor cell growth in peritoneal cell cultures from tumor-dormant mice.

作者信息

Suzuki Y, Liu C M, Chen L P, Ben-Nathan D, Wheelock E F

机构信息

Department of Pathology and Laboratory Medicine, Hahnemann University, Philadelphia, PA 19102.

出版信息

J Immunol. 1987 Nov 1;139(9):3146-52.

PMID:3117888
Abstract

L5178Y lymphoma cells are restrained from progressive growth in peritoneal cell ("in vitro tumor-regressor" PC) cultures prepared from many DBA/2 mice which harbor the tumor cells in the peritoneal cavity in a tumor-dormant state. Treatment of these PC cultures with 'antibodies to murine interferon-gamma (MuIFN-gamma) and murine tumor necrosis factor (MuTNF) but not with antibody to interleukin 2 (IL-2) receptors eliminated the restraint on tumor cell growth and permitted their progressive proliferation. L5178Y cells were found to be resistant to the direct toxic effects of large concentrations (3,000 U/ml) of MuIFN-gamma and of MuTNF, either alone or in combination. Treatment of PC cultures from tumor-dormant mice, in which tumor cells grew progressively ("in vitro tumor-progressor"), but not PC cultures from normal mice, with exogenous MuIFN-gamma resulted in a marked inhibition of tumor cell growth. The MuIFN-gamma-induced cytotoxic activity was cell-mediated since no soluble tumor-cytotoxic factors could be detected in the cultures. MuIFN-gamma induced cytotoxic activity in plastic-adherent peritoneal cell (AD-PC) cultures, but induced no cytotoxic activity in nonadherent-PC cultures unless small numbers (2%) of AD-PC were present, and inclusion of antibody to MuTNF in these mixed PC cultures blocked the development of cytotoxic activity. Antibody to MuTNF also blocked the development of cytotoxic activity in cultures of MuIFN-gamma-treated whole PC and AD-PC from tumor-dormant mice. These results indicate that MuIFN-gamma and MuTNF are both important in restraining tumor cell growth in PC cultures from tumor-dormant mice, and that MuIFN-gamma requires the presence of MuTNF to induce cytotoxic activity in these cultures.

摘要

L5178Y淋巴瘤细胞在从许多DBA/2小鼠制备的腹膜细胞(“体外肿瘤抑制细胞”PC)培养物中受到抑制,无法进行渐进性生长,这些小鼠的腹腔中以肿瘤休眠状态携带肿瘤细胞。用抗小鼠干扰素-γ(MuIFN-γ)和抗小鼠肿瘤坏死因子(MuTNF)抗体处理这些PC培养物,但不用抗白细胞介素2(IL-2)受体抗体处理,可消除对肿瘤细胞生长的抑制,并使其进行性增殖。发现L5178Y细胞对高浓度(3000 U/ml)的MuIFN-γ和MuTNF单独或联合的直接毒性作用具有抗性。用外源性MuIFN-γ处理来自肿瘤休眠小鼠的PC培养物(其中肿瘤细胞进行性生长,即“体外肿瘤促进细胞”),而不是来自正常小鼠的PC培养物,会导致肿瘤细胞生长受到明显抑制。MuIFN-γ诱导的细胞毒性活性是细胞介导的,因为在培养物中未检测到可溶性肿瘤细胞毒性因子。MuIFN-γ在塑料贴壁腹膜细胞(AD-PC)培养物中诱导细胞毒性活性,但在非贴壁PC培养物中不诱导细胞毒性活性,除非存在少量(2%)的AD-PC,并且在这些混合PC培养物中加入抗MuTNF抗体可阻断细胞毒性活性的发展。抗MuTNF抗体也可阻断MuIFN-γ处理的来自肿瘤休眠小鼠的全PC和AD-PC培养物中细胞毒性活性的发展。这些结果表明,MuIFN-γ和MuTNF在抑制来自肿瘤休眠小鼠的PC培养物中肿瘤细胞生长方面都很重要,并且MuIFN-γ需要MuTNF的存在才能在这些培养物中诱导细胞毒性活性。

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