[Effects of perinatal exposure to the brominated flame-retardant hexabromocyclododecane (HBCD) on the developing immune system in rats].

Q4 Medicine
Akiko Hachisuka, Ryosuke Nakamura, Yuji Sato, Rika Nakamura, Makoto Shibutani, Reiko Teshima
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引用次数: 0

Abstract

To evaluate the developmental immunotoxicity of brominated flame retardant, hexabromocyclododecane (HBCD) , maternal Sprague-Dawley rats were given HBCD at dietary concentrations of 0, 100, 1000, 10000 ppm from gestational day 10 to postnatal day 21 (postnatal week 3, PNW3). At PNW3 and PNW11, lymphocytes in the spleen, thymus, and peripheral blood of male pups were subjected to flow cytometric analyses for expression of surface markers (CD3, CD4, CD8a, CD25, CD45RA, CD71, and CD161 (NKRP1A)). The spleen and thymus weights, and number of white blood cells of two organs did not change between HBCD-exposed and control groups at PNW3 and PNW11. A significant decrease in thyroid hormone T3 and increase in serum albumin concentration were observed at PNW3 and lasted until PNW11. By flow cytometric analysis, the dramatic change was not observed in the population of the splenic and thymic T/B lymphocyte between the HBCD treated groups and control group. In the peripheral blood of BNW3 rats, the population of activated T cells was decreased and that of inactivated B cells was increased. And the population of NK cells in the spleen was decreased. All of these changes were mild in degree, and returned to the normal levels by PNW11. Production of anti-KLH IgG antibody after KLH immunization was reduced by the 10000 ppm HBCD treatment. These results suggest that developmental exposure to the highest dose of HBCD had a weak immunomodulatory effect at PNW3, and most of the immunomodulatory effect had recovered to normal levels by PNW11.

[围产期接触溴化阻燃剂六溴环十二烷(HBCD)对大鼠发育中的免疫系统的影响]。
为了评价溴化阻燃剂六溴环十二烷(HBCD)的发育免疫毒性,从妊娠第10天至出生后第21天(出生后第3周,PNW3),母体Sprague-Dawley大鼠在饮食中分别给予浓度为0、100、1000和10000 ppm的HBCD。在PNW3和PNW11时,用流式细胞术分析雄性幼崽脾脏、胸腺和外周血中的淋巴细胞表达表面标记物(CD3、CD4、CD8a、CD25、CD45RA、CD71和CD161 (NKRP1A))。在PNW3和PNW11时,hbcd暴露组和对照组的脾脏和胸腺重量以及两个器官的白细胞数量没有变化。在PNW3时,甲状腺激素T3显著降低,血清白蛋白浓度升高,并持续到PNW11。通过流式细胞术分析,在治疗组和对照组之间没有观察到脾脏和胸腺T/B淋巴细胞数量的显著变化。BNW3大鼠外周血中活化的T细胞数量减少,灭活的B细胞数量增加。脾脏NK细胞数量减少。所有这些变化在程度上都是轻微的,并在PNW11后恢复到正常水平。10000 ppm HBCD处理可降低KLH免疫后抗KLH IgG抗体的产生。这些结果表明,发育过程中暴露于最高剂量的HBCD对PNW3的免疫调节作用较弱,大部分免疫调节作用在PNW11后恢复到正常水平。
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