Effects of Fumonisin B1on the Immune System of Sprague–Dawley Rats Following a 14-Day Oral (Gavage) Exposure

H. Tryphonas , G. Bondy , J.D. Miller , F. Lacroix , M. Hodgen , P. Mcguire , S. Fernie , D. Miller , S. Hayward
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Abstract

The effects of fumonisin B1(FB1) on the immune system of Sprague–Dawley rats were investigated. Groups of male and female rats (10 rats/group) were gavaged daily for 14 days with doses of 0, 5, 15, and 25 mg/kg body wt/day and the primary (IgM) response to sheep red blood cells expressed as plaque-forming cell numbers/106spleen mononuclear leukocytes (PFC/106splenocytes) and PFC/spleen was determined. There was a significant dose-related linear trend toward decreased PFC/106splenocytes (p= 0.003) and PFC/spleen cells (p= 0.001) in the male rats. Body weights, expressed as a percentage of the control, were significantly reduced (p= 0.002) in the male rats administered 15 and 25 mg/kg doses. The PFC numbers in female rats were not affected significantly by treatment (p> 0.05). For the remaining immunotoxicity studies, groups of male rats (10 rats/group) were gavaged with FB1doses of 0, 1, 5, and 15 mg/kg body wt/day for 14 days. There was a weakly significant dose-related trend toward increased numbers of serum immunoglobulin class G (p= 0.04). Also a significant dose-related increase (p= 0.013) inListeria monocytogenesnumbers was observed in the spleen at 24 hr postinfection. Treatment did not have a significant effect on organ weights, hematology, mitogen-induced lymphocyte transformation, calcium mobilization, the numbers of leukocytes and T-lymphocyte subsets, the natural killer cell activity, and phagocytosis (p≥ 0.05). These observations suggested that FB1may have indirect consequences for human health and warrant further investigations.

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伏马菌素b1对Sprague-Dawley大鼠灌胃14天后免疫系统的影响
研究伏马菌素B1(FB1)对Sprague-Dawley大鼠免疫系统的影响。各组雄性和雌性大鼠(10只/组)每天以0、5、15和25 mg/kg体重量/天的剂量灌胃14天,测定其对以斑块形成细胞数/106脾脏单核白细胞(PFC/106脾脏细胞)和PFC/脾脏表达的绵羊红细胞的初级(IgM)反应。雄性大鼠PFC/106脾细胞和PFC/脾细胞呈显著的剂量相关线性下降趋势(p= 0.003)。在15和25 mg/kg剂量的雄性大鼠中,体重(以对照的百分比表示)显著降低(p= 0.002)。雌性大鼠的PFC数量未受治疗的显著影响(p>0.05)。在其余免疫毒性研究中,雄性大鼠各组(10只/组)分别以0、1、5和15 mg/kg体重量/天的剂量灌胃fb1,持续14天。血清免疫球蛋白G类增加呈弱显著剂量相关趋势(p= 0.04)。感染后24小时,脾脏单核细胞增生李斯特菌数量也有显著的剂量相关增加(p= 0.013)。治疗对器官重量、血液学、丝裂原诱导的淋巴细胞转化、钙动员、白细胞和t淋巴细胞亚群数量、自然杀伤细胞活性和吞噬能力均无显著影响(p≥0.05)。这些观察结果表明,fb1可能对人类健康产生间接影响,值得进一步调查。
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