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氧化双(三正丁基锡)对大鼠的毒性。II. 短期暴露后对胸腺依赖性免疫反应和非特异性抵抗力参数的抑制作用。

Toxicity of bis(tri-n-butyltin)oxide in the rat. II. Suppression of thymus-dependent immune responses and of parameters of nonspecific resistance after short-term exposure.

作者信息

Vos J G, de Klerk A, Krajnc E I, Kruizinga W, van Ommen B, Rozing J

出版信息

Toxicol Appl Pharmacol. 1984 Sep 30;75(3):387-408. doi: 10.1016/0041-008x(84)90177-7.

DOI:10.1016/0041-008x(84)90177-7
PMID:6474470
Abstract

To evaluate the functional significance of bis(tri-n-butyltin)oxide (TBTO)-induced thymus atrophy, lymphocyte depletion in spleen and lymph nodes, lymphopenia, and increased serum IgM and decreased IgG concentrations, in vivo and in vitro function studies were performed for specific and nonspecific resistance. Weaned male rats were fed diets containing 0, 20, or 80 mg TBTO/kg for at least 6 weeks. Regarding the thymus-dependent immunity, delayed-type hypersensitivity reactions to ovalbumin as well as tuberculin were significantly depressed at both dietary concentrations. Resistance to the nematode Trichinella spiralis was significantly suppressed as shown by a retarded expulsion of adult worms from the small intestine, increased counts of muscle larvae, reduced inflammatory reaction in parasitized musculature, and suppressed serum IgE titers. Also the secondary mercaptoethanol-resistant (presumably IgG) hemagglutinating antibody titer to sheep red blood cells was significantly reduced, while no significant alterations were found in IgM and IgG titers to T. spiralis, ovalbumin, and tetanus toxoid. TBTO exposure reduced the response of thymocytes in both treatment groups and of spleen cells in the 80-mg/kg group upon stimulation with T-cell mitogens and increased the response of spleen cells to B-cell mitogens. When calculated per whole spleen, the response to T-cell mitogens was strongly impaired but unaltered by B-cell mitogens. This difference can be explained by a relative increase of splenic B cells as a result of reduced numbers of T cells, as shown by cell surface marker analysis using monoclonal antibodies. Reduced splenic T-cell numbers appeared equally due to a decreased number of T helper and to T suppressor cells. From these data and from results of a time-sequence study in which effects of TBTO on cell count and cell viability of thymus, spleen, and bone marrow were investigated, it is concluded that TBTO-induced immunodeficiency was primarily due to its direct toxic action on thymocytes. When cultured in vitro in the presence of TBTO, viability of thymus and bone marrow cells was equally reduced, while after in vivo treatment viability of bone marrow cells was unaffected. Thus, the in vitro situation does not mimic the in vivo one. Concerning the nonspecific resistance, TBTO reduced macrophage function as shown by impaired splenic clearance of Listeria monocytogenes bacteria. From in vitro studies it is concluded that impaired in vivo splenic clearance was due to a reduction in both the number of adherent cells in the spleen and bacterial digestion on a cell for cell basis.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

为评估双(三正丁基锡)氧化物(TBTO)诱导的胸腺萎缩、脾脏和淋巴结淋巴细胞减少、淋巴细胞减少以及血清IgM升高和IgG浓度降低的功能意义,进行了体内和体外特异性及非特异性抵抗力的功能研究。将断奶雄性大鼠喂食含0、20或80mg TBTO/kg的饲料至少6周。关于胸腺依赖性免疫,在两种饮食浓度下,对卵清蛋白以及结核菌素的迟发型超敏反应均显著降低。对旋毛虫线虫的抵抗力显著受到抑制,表现为成虫从小肠排出延迟、肌肉幼虫数量增加、寄生肌肉组织中的炎症反应减轻以及血清IgE滴度降低。此外,对绵羊红细胞的二级巯基乙醇抗性(可能是IgG)血凝抗体滴度也显著降低,而对旋毛虫、卵清蛋白和破伤风类毒素的IgM和IgG滴度未发现显著变化。TBTO暴露降低了两个治疗组胸腺细胞以及80mg/kg组脾脏细胞在用T细胞有丝分裂原刺激后的反应,并增加了脾脏细胞对B细胞有丝分裂原的反应。按整个脾脏计算,对T细胞有丝分裂原的反应严重受损,但对B细胞有丝分裂原的反应未改变。这种差异可以通过T细胞数量减少导致脾脏B细胞相对增加来解释,这通过使用单克隆抗体的细胞表面标志物分析得以证明。脾脏T细胞数量减少同样是由于T辅助细胞和T抑制细胞数量减少。从这些数据以及一项时间序列研究的结果(该研究调查了TBTO对胸腺、脾脏和骨髓细胞计数及细胞活力的影响)可以得出结论,TBTO诱导的免疫缺陷主要是由于其对胸腺细胞的直接毒性作用。当在TBTO存在下体外培养时,胸腺和骨髓细胞的活力同样降低,而体内治疗后骨髓细胞的活力未受影响。因此,体外情况并不能模拟体内情况。关于非特异性抵抗力,TBTO降低了巨噬细胞功能,表现为脾脏对单核细胞增生李斯特菌细菌的清除受损。从体外研究可以得出结论,体内脾脏清除受损是由于脾脏中黏附细胞数量减少以及细胞对细胞的细菌消化减少。(摘要截取自400字)

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