拟胸腺药物和补锌对氢化可的松抑制小鼠细胞免疫反应的影响。

B Obmińska-Domoradzka, M Szczypka, J Debowy
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引用次数: 9

摘要

该研究是在Balb/c小鼠(5-6周龄)上进行的,暴露于单次腹腔剂量(125 mg/kg)氢化可的松免疫抑制。在注射氢化可的松之前,小鼠腹腔注射二乙基二硫代氨基甲酸乙酯(DTC),剂量为20 mg/kg,间隔48 h 5次,或小牛胸腺提取物(TFX),剂量为10 mg/kg,间隔24 h 10次。这两种药物单独使用或在锌离子相互作用中使用,通过在饮用水中添加锌离子(作为硫酸盐),剂量为每天72微克/只小鼠。本研究结果显示,氢化可的松注射使胸腺细胞和脾细胞数量明显减少,胸腺和脾脏的重量比也随之下降。胸腺和脾脏细胞数量的减少与CD4+、CD8+和CD19+脾细胞和双阳性CD4+CD8+胸腺细胞百分比的减少相对应。胸腺细胞数量的变化会影响它们的活性,这表现为胸腺细胞在体外受豆豆蛋白a (Con a)和植物血凝素(PHA)刺激时的增殖反应降低。研究还发现,在体外用大肠杆菌脂多糖刺激小鼠腹腔巨噬细胞时,单次氢化可的松剂量可减少白细胞介素(IL)-1的产生。TFX或DTC可抵消氢化可的松诱导的免疫抑制,其表现为胸腺和脾脏细胞总数部分正常化,加速两个淋巴器官的再生,缩短氢化可的松对CD4+、CD8+脾细胞和双阳性(CD4+CD8+)和CD4+胸腺细胞百分比的抑制作用。此外,我们还观察到氢化可的松对Con A和PHA体外刺激胸腺细胞增殖活性的抑制作用完全被抵消。在注射氢化可的松之前给药TFX部分阻止了药物对腹腔巨噬细胞IL-1产生的抑制作用,但DTC没有观察到这种作用。补锌可增强TFX和DTC的免疫恢复作用。研究结果表明,无论是TFX还是DTC给药本身,以及与锌补充的相互作用,都不能改变氢化可的松对B脾细胞(CD19+细胞)百分比的抑制作用。
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Effects of thymomimetic drugs and zinc supplementation on the cellular immune response in hydrocortisone-suppressed mice.

The studies were carried out on Balb/c mice (5-6 weeks of age) exposed to immunosuppression by a single intraperitoneal dose (125 mg/kg) of hydrocortisone. Prior to hydrocortisone injection the mice were treated with diethyldithiocarbamate (DTC) intra-peritoneally at a dose of 20 mg/kg, five times at 48 h intervals or calf thymus extract (TFX) at a dose of 10 mg/kg, 10 times at 24 h intervals. The two drugs were used per se or in zinc ions interactions, by adding zinc ions (as sulphate salt) to drinking water at a dose of 72 microg/mouse per day. The results obtained in the study show that hydrocortisone injection drastically decreases the number of thymocytes and splenocytes, which is also accompanied by a decreasing weight ratio of the thymus and spleen. The decreasing number of thymic and spleen cells corresponds to a decreasing percentage of CD4+, CD8+ and CD19+ splenocytes and double positive CD4+CD8+ thymocytes. Changes in the number of thymic cells affect their activity, which is expressed in a decreased proliferative response of thymocytes stimulated in vitro with concanavalin A (Con A) and phytohaemagglutinin (PHA). It has also been found that a single hydrocortisone dose decreases interleukin (IL)-1 production by murine intraperitoneal macrophages stimulated in vitro with lipopolysaccharide (LPS) from Escherichia coli. TFX or DTC counteract hydrocortisone-induced immunosuppression, which is expressed in partial normalization of the total number of thymic and spleen cells, accelerated regeneration of the two lymphatic organs, shorter suppressive action of hydrocortisone on the percentage of CD4+, CD8+ splenocytes and double positive (CD4+CD8+) and CD4+ thymocytes. Furthermore, total counteraction against the suppressive action of hydrocortisone to proliferative activity of thymocytes stimulated in vitro with Con A and PHA was observed. TFX administered prior to hydrocortisone injection partially prevented the suppressive action of the drug on IL-1 production by intraperitoneal macrophages, but such an effect was not observed with DTC. The immunorestorative effect of TFX and DTC was augmented by zinc supplementation. The results obtained in the study show that neither TFX nor DTC administration per se and in interaction with zinc supplementation were able to change the suppressive effect of hydrocortisone on the percentage of B splenocytes (CD19+ cells).

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