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美国红隼(Falco sparverius)摄入十溴二苯醚(BDE-209)阻燃剂的饮食暴露:摄取、分布、脱溴和细胞色素 P450 酶诱导。

Dietary exposure of American kestrels (Falco sparverius) to decabromodiphenyl ether (BDE-209) flame retardant: uptake, distribution, debromination and cytochrome P450 enzyme induction.

机构信息

Ecotoxicology and Wildlife Health Division, Science and Technology Branch, Environment Canada, Ottawa, Ontario K1A 0H3, Canada.

Avian Science and Conservation Centre, Department of Natural Resource Sciences, McGill University, Ste-Anne-de-Bellevue, Quebec, Canada.

出版信息

Environ Int. 2014 Feb;63:182-90. doi: 10.1016/j.envint.2013.11.010. Epub 2013 Dec 4.

DOI:10.1016/j.envint.2013.11.010
PMID:24317224
Abstract

Accumulation and evidence of debromination of the flame retardant 2,2',3,3',4,4',5,5',6,6'-decabromodiphenyl ether (BDE-209) have been reported for biota, including raptorial birds, based on PBDE congener residues in tissues and eggs. However, in vivo studies with BDE-209-exposed birds are rare and unknown for a raptorial species. In the present study, males (n=22) of raptorial American kestrels (Falco sparverius) were exposed to 116,000ng of BDE-209 (high purity, >98%; in safflower oil) per day for 21days (~2,436,000ng total BDE-209 exposure over this uptake period), followed by a 25-day depuration period. Control males (n=11) received the safflower vehicle only. In the exposed birds, BDE-209 was quantifiable in all plasma (end of uptake and depuration period) as well as liver and fat (end of depuration only) samples. The mean (±SE) BDE-209 level in plasma was 1474±1145ng/g wet weight (ww) at the end of the uptake period, and was significantly (p<0.001) lower (88%) at 174±148ng/g ww after the 25day depuration period. This equates to a mean reduction rate of 52ng/g ww per day and a rough estimation of the BDE-209 half-life in plasma of approximately 14days. The mean (±SE) BDE-209 levels were 4668±6192ng/g ww in the fat, and 338±311ng/g ww in the liver, of exposed individuals, which were significantly (p≤0.001) greater than mean concentrations (25±20 in fat and 2.6±0.9ng/g ww in liver) in the control birds. In addition to BDE-209, lower brominated PBDE congeners, and mainly meta- and para-debromination products of BDE-209 were also quantified in plasma, liver and/or fat. We estimated based on the dose that at least 80% of the non-BDE-209 concentration in the kestrel tissues and plasma must be derived from BDE-209 debromination by the kestrels. Where quantifiable, lower brominated PBDE concentrations were significantly (0.023>p>0.001) higher in the exposed relative to the control bird samples (except for BDE-154 and -153 in fat). Additional PBDE congeners found in plasma included nona-BDEs (208, 207 and 206), followed by octa-BDEs (197, 196, 201 and 203), and in liver and/or fat, the hepta-BDEs 180 and 183 and BDE-153. Higher hepatic EROD activity (cytochrome P450 1A1 monooxygenase-mediation) in the exposed birds compared to control birds was strongly suggested to be PBDE-induced, and was consistent with BDE-209 and congener metabolism in the exposed kestrels. The mean EROD activity rate was 36.1pmol/min/mg protein relative to the (n=4) control birds whose activity was just above the detection limit (10.3pmol/min/mg protein). Overall, the results demonstrated that following diet exposure of kestrels to high purity BDE-209, uptake occurred as well as BDE-209 degradation via debromination to lower brominated PBDE congeners.

摘要

生物体内(包括猛禽)已经发现了阻燃剂 2,2',3,3',4,4',5,5',6,6'-十溴二苯醚(BDE-209)的积累和去溴化证据,这些证据基于组织和卵中的多溴二苯醚同系物残留。然而,在摄入 BDE-209 的鸟类体内进行的体内研究非常罕见,特别是针对猛禽物种。在本研究中,雄性美洲红隼(Falco sparverius)(n=22)每天暴露于 116,000ng 的 BDE-209(高纯度,>98%;红花油中),为期 21 天(在这段吸收期内总共摄入 2,436,000ng 的 BDE-209),随后进行 25 天的清除期。对照组雄性(n=11)仅接受红花油载体。在暴露组的所有血浆(吸收和清除期结束时)以及肝脏和脂肪(仅清除期结束时)样本中都可以定量 BDE-209。在吸收期结束时,暴露组血浆中 BDE-209 的平均(±SE)水平为 1474±1145ng/g 湿重(ww),在 25 天的清除期后,显著(p<0.001)降低(88%)至 174±148ng/g ww。这相当于每天减少 52ng/g ww 的平均下降率,以及大约 14 天的 BDE-209 血浆半衰期的粗略估计。暴露个体的脂肪中 BDE-209 的平均(±SE)水平为 4668±6192ng/g ww,肝脏中为 338±311ng/g ww,显著(p≤0.001)高于对照组鸟类的平均浓度(脂肪中 25±20,肝脏中 2.6±0.9ng/g ww)。除了 BDE-209 之外,还在血浆、肝脏和/或脂肪中定量了较低溴化的多溴二苯醚同系物,主要是 BDE-209 的间位和对位去溴化产物。我们根据剂量估计,猛禽组织和血浆中至少 80%的非 BDE-209 浓度必须来自猛禽的 BDE-209 去溴化作用。在所定量的情况下,暴露组相对于对照组鸟类样本,较低溴化的多溴二苯醚浓度显著(0.023>p>0.001)升高(脂肪中除 BDE-154 和 -153 外)。在血浆中发现的其他多溴二苯醚同系物包括九溴二苯醚(208、207 和 206),其次是八溴二苯醚(197、196、201 和 203),以及在肝脏和/或脂肪中,七溴二苯醚 180 和 183 和 BDE-153。暴露组鸟类的肝脏 EROD 活性(细胞色素 P450 1A1 单加氧酶介导)明显高于对照组鸟类,这强烈表明是 PBDE 诱导的,与暴露的红隼中 BDE-209 和同系物代谢一致。暴露组的平均 EROD 活性率为 36.1pmol/min/mg 蛋白,而对照组(n=4)鸟类的活性刚刚高于检测限(10.3pmol/min/mg 蛋白)。总体而言,研究结果表明,在红隼通过饮食暴露于高纯度 BDE-209 后,既发生了 BDE-209 的摄取,也发生了 BDE-209 通过去溴化作用降解为较低溴化的多溴二苯醚同系物。

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