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狄氏剂对MHV3病毒激活的巨噬细胞的抑制作用。

Suppression of MHV3 virus-activated macrophages by dieldrin.

作者信息

Krzystyniak K, Bernier J, Hugo P, Fournier M

出版信息

Biochem Pharmacol. 1986 Aug 1;35(15):2577-86. doi: 10.1016/0006-2952(86)90056-0.

Abstract

Dieldrin (36 mg/kg body weight) administered intraperitoneally prolonged recovery from infection with mouse hepatitis virus 3 (MHV3) in the genetically-resistant A/J strain, affected the humoral anti-MHV3 IgG immune response, and inhibited the intrinsic antiviral activity of peritoneal macrophages upon in vitro rechallenge with the virus. Infection of untreated A/J animals and vehicle controls with MHV3 resulted in marked and reproducible activation of peritoneal macrophages, observed in vitro as resistance to MHV3-cytopathic effects 48 hr after rechallenge with the virus, whereas exposure to dieldrin resulted in apparent loss of the intrinsic capacity of cells to restrict replication of MHV3 and to protect them from cytolysis. In addition, in vitro treatment of MHV3 virus-activated macrophages with dieldrin, mitomycin C and X-irradiation, inhibited the intrinsic capacity of cells to restrict MHV3 replication. This mechanism of cellular restriction of the virus by MHV3-activated macrophages from the resistant A/J strain appeared to be one of the sensitive targets for the suppressive action of dieldrin on host resistance, as no major changes in macrophage cellular parameters were observed in in vitro studies of cell viability, adherence to plastic, and superoxide anion generation; the increased cell yield in the peritoneal exudates during MHV3 virus infection was not affected by dieldrin exposure; and the attachment and uptake of [3H]MHV3 by virus-activated macrophages was shown to be unchanged by dieldrin exposure.

摘要

腹腔注射狄氏剂(36毫克/千克体重)可延长基因抗性A/J品系小鼠感染小鼠肝炎病毒3型(MHV3)后的恢复时间,影响体液中抗MHV3 IgG免疫反应,并在病毒体外再次攻击时抑制腹腔巨噬细胞的固有抗病毒活性。用MHV3感染未处理的A/J动物和溶剂对照组,会导致腹腔巨噬细胞显著且可重复的激活,在病毒再次攻击48小时后,体外观察到其对MHV3细胞病变效应具有抗性,而接触狄氏剂会导致细胞限制MHV3复制并保护自身免受细胞溶解的固有能力明显丧失。此外,用狄氏剂、丝裂霉素C和X射线对MHV3病毒激活的巨噬细胞进行体外处理,会抑制细胞限制MHV3复制的固有能力。来自抗性A/J品系的MHV3激活巨噬细胞对病毒的这种细胞限制机制似乎是狄氏剂对宿主抗性抑制作用的敏感靶点之一,因为在细胞活力、对塑料的黏附以及超氧阴离子生成的体外研究中未观察到巨噬细胞细胞参数的重大变化;MHV3病毒感染期间腹腔渗出液中细胞产量的增加不受狄氏剂暴露的影响;并且狄氏剂暴露显示病毒激活的巨噬细胞对[3H]MHV3的附着和摄取未发生变化。

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本文引用的文献

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Radioimmunoassays of hidden viral antigens.隐匿性病毒抗原的放射免疫测定
Proc Natl Acad Sci U S A. 1982 Jul;79(14):4415-9. doi: 10.1073/pnas.79.14.4415.

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