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氯脲霉素,一种在治疗剂量下无骨髓毒性的抗肿瘤药物:对小鼠淋巴细胞亚群的影响。

Chlorozotocin, an anti-tumour agent lacking bone marrow toxicity at therapeutic doses: effects on lymphocyte subpopulations in mice.

作者信息

Fisher R I, Mandell G L, Bostick F, McMenamin M G, Anderson T

出版信息

Clin Exp Immunol. 1980 Feb;39(2):416-25.

Abstract

Chlorozotocin is a new nitrosourea anti-tumour drug that does not produce bone marrow suppression at therapeutic doses in mice. CDF1 mice which were injected i.p. with a dose lethal to 10% of animals within 60 days (LD10), 20 mg/kg, developed a 50% reduction in circulating peripheral blood lymphocytes without a decrease in circulating granulocytes by day 3. Spleen weight also decreased markedly. The percentage of spleen B and T cells, determined by immunofluorescence with goat anti-mouse IgG and rabbit anti-mouse brain antisera, did not differ in control and chlorozotocin-treated mice. However, the ability of residual spleen cells to proliferate in response to phytohaemagglutinin, concanavalin A, pokeweed mitogen, and allogeneic cells was significantly suppressed although the lipopolysaccharide response was not reduced. The ability of the mice to respond to a primary immunization with sheep red blood cells was not significantly impaired. Therefore, chlorozotocin has a cytotoxic effect on both B and T cells but selectively inhibits the proliferative capacity of T cells. B cell proliferation and B cell function as measured in a primary antibody response were not reduced. These studies suggest chlorozotocin may be useful as an immunosuppressive drug as well as an anti-tumour agent.

摘要

氯脲霉素是一种新型亚硝基脲类抗肿瘤药物,在小鼠治疗剂量下不会产生骨髓抑制。给CDF1小鼠腹腔注射20mg/kg剂量,该剂量在60天内对10%的动物致死(LD10),到第3天时,循环外周血淋巴细胞减少50%,而循环粒细胞数量未减少。脾脏重量也显著下降。用山羊抗小鼠IgG和兔抗小鼠脑抗血清通过免疫荧光法测定,对照小鼠和氯脲霉素处理小鼠的脾脏B细胞和T细胞百分比没有差异。然而,尽管脂多糖反应未降低,但残留脾细胞对植物血凝素、刀豆蛋白A、商陆有丝分裂原和同种异体细胞增殖的能力受到显著抑制。小鼠对绵羊红细胞初次免疫的反应能力没有明显受损。因此,氯脲霉素对B细胞和T细胞均有细胞毒性作用,但选择性抑制T细胞的增殖能力。在初次抗体反应中测得的B细胞增殖和B细胞功能未降低。这些研究表明氯脲霉素可能作为一种免疫抑制药物以及抗肿瘤药物有用。

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