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镉对孕鼠的急性毒性和致畸性。

The acute toxicity and teratogenicity of cadmium in the pregnant rat.

作者信息

Samarawickrama G P, Webb M

出版信息

J Appl Toxicol. 1981 Oct;1(5):264-9. doi: 10.1002/jat.2550010506.

DOI:10.1002/jat.2550010506
PMID:7185887
Abstract

Until the 16th day of gestation the intravenous LD50 of Cd2+ in the pregnant Wistar-Porton rat is higher, but not significantly different from that (1.8 mg Cd2+ per kg body weight) in nulliparous females. At 20 days it is 1.1 mg Cd2+ kg per body weight. This decrease is related to the rapid increase in weight of the conceptuses in late gestation and to the retention of most of the dose in the maternal compartment. If the dose is based on body weight at conception, the LD50 for the 20-day pregnant rat (1.6 mg Cd2+ per kg body weight) and non-gravid female do not differ significantly. Nevertheless, after the same Cd2+ dose, hepatic and renal Cd2+ concentrations are less in the pregnant than in the non-pregnant animal. The Cd2+ concentrations, therefore, do not determine the liver and kidney damage, which is restricted to the pregnant rat. Placentae also accumulate Cd2+ and placental haemorrhage follows the injection of the appropriate Cd2+ LD50 on day 12-20 of gestation. In those animals that die between 16 and 30 h after dosing, haemorrhage and death appear to be correlated. Renal damage, therefore, probably results from haemorrhagic shock. It is not dependent on the transfer of protein-bound Cd2+ from the necrotic placentae to the kidney. Between the 8th and 15th day of gestation, Cd2+ (1.25 mg per kg body weight) is highly teratogenic. Hydrocephalus is the most frequent abnormality when the dose is given between the 8th and 12th day. Other malformations include eye defects, gastroschiasis and umbilical hernia.

摘要

在妊娠第16天之前,妊娠Wistar-Porton大鼠静脉注射Cd2+的半数致死剂量(LD50)较高,但与未孕雌性大鼠的LD50(每千克体重1.8毫克Cd2+)无显著差异。在妊娠20天时,LD50为每千克体重1.1毫克Cd2+。这种降低与妊娠后期胎儿体重的快速增加以及大部分剂量保留在母体部分有关。如果剂量基于受孕时的体重,20天妊娠大鼠的LD50(每千克体重1.6毫克Cd2+)与未孕雌性大鼠无显著差异。然而,给予相同剂量的Cd2+后,妊娠大鼠肝脏和肾脏中的Cd2+浓度低于未孕动物。因此,Cd2+浓度并不能决定仅限于妊娠大鼠的肝脏和肾脏损伤。胎盘也会积累Cd2+,在妊娠第12 - 20天注射适当的Cd2+ LD50后会出现胎盘出血。在给药后16至30小时内死亡的动物中,出血与死亡似乎相关。因此,肾脏损伤可能是由失血性休克导致的。它不依赖于与蛋白质结合的Cd2+从坏死胎盘转移至肾脏。在妊娠第8天至15天期间,Cd2+(每千克体重1.25毫克)具有高度致畸性。当在第8天至12天给药时,脑积水是最常见的异常情况。其他畸形包括眼部缺陷、腹裂和脐疝。

相似文献

1
The acute toxicity and teratogenicity of cadmium in the pregnant rat.镉对孕鼠的急性毒性和致畸性。
J Appl Toxicol. 1981 Oct;1(5):264-9. doi: 10.1002/jat.2550010506.
2
Acute effects of cadmium on the pregnant rat and embryo-fetal development.镉对孕鼠及胚胎-胎儿发育的急性影响。
Environ Health Perspect. 1979 Feb;28:245-9. doi: 10.1289/ehp.7928245.
3
Teratogenicity, fetal toxicity and tissue concentration of cadmium administered to female rats during organogenesis.器官形成期给雌性大鼠施用镉的致畸性、胎儿毒性及组织浓度
J Appl Toxicol. 1982 Oct;2(5):255-9. doi: 10.1002/jat.2550020508.
4
The toxicity and teratogenicity of mercuric mercury in the pregnant rat.汞对怀孕大鼠的毒性和致畸性。
Arch Toxicol. 1986 Apr;58(4):243-8. doi: 10.1007/BF00297114.
5
Teratogenicity of ionic cadmium in the Wistar rat.离子镉对Wistar大鼠的致畸性。
Arch Toxicol. 1987 Apr;59(6):443-7. doi: 10.1007/BF00316212.
6
Placental transport and embryonic utilization of essential metabolites in the rat at the teratogenic dose of cadmium.镉致畸剂量下大鼠体内必需代谢物的胎盘转运及胚胎利用情况
J Appl Toxicol. 1981 Oct;1(5):270-7. doi: 10.1002/jat.2550010507.
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Comparison of some biochemical effects of teratogenic doses of mercuric mercury and cadmium in the pregnant rat.致畸剂量的汞和镉对孕鼠某些生化效应的比较。
Arch Toxicol. 1986 Apr;58(4):249-54. doi: 10.1007/BF00297115.
8
The teratogenicity of cadmium-metallothionein in the rat.大鼠中镉-金属硫蛋白的致畸性。
Arch Toxicol. 1988;61(6):457-67. doi: 10.1007/BF00293692.
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Teratogenic effects and distribution of cadmium (Cd2+) administered via osmotic minipumps to gravid CF-1 mice.通过渗透微型泵给妊娠CF-1小鼠注射镉离子(Cd2+)的致畸作用及分布情况。
Toxicol Lett. 1995 Apr;76(3):195-202. doi: 10.1016/0378-4274(95)80003-v.
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A morphological and biochemical study of the effects of L-cysteine on the renal uptake and nephrotoxicity of cadmium.L-半胱氨酸对镉的肾脏摄取及肾毒性影响的形态学与生物化学研究
Br J Exp Pathol. 1981 Apr;62(2):115-30.

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Gestational cadmium exposure-induced ovotoxicity delays puberty through oxidative stress and impaired steroid hormone levels.妊娠期镉暴露诱导的卵母细胞毒性通过氧化应激和类固醇激素水平降低来延迟青春期。
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Teratogens inducing congenital abdominal wall defects in animal models.
在动物模型中诱导先天性腹壁缺陷的致畸剂。
Pediatr Surg Int. 2010 Feb;26(2):127-39. doi: 10.1007/s00383-009-2482-z. Epub 2009 Sep 16.
4
Effect of progesterone pretreatment on cadmium toxicity in male Fischer (F344/NCr) and Wistar (WF/NCr) rats.孕酮预处理对雄性Fischer(F344/NCr)和Wistar(WF/NCr)大鼠镉毒性的影响。
Environ Health Perspect. 1994 Sep;102 Suppl 3(Suppl 3):277-80. doi: 10.1289/ehp.94102s3277.
5
Comparison of some biochemical effects of teratogenic doses of mercuric mercury and cadmium in the pregnant rat.致畸剂量的汞和镉对孕鼠某些生化效应的比较。
Arch Toxicol. 1986 Apr;58(4):249-54. doi: 10.1007/BF00297115.
6
The toxicity and teratogenicity of mercuric mercury in the pregnant rat.汞对怀孕大鼠的毒性和致畸性。
Arch Toxicol. 1986 Apr;58(4):243-8. doi: 10.1007/BF00297114.
7
Teratogenicity of ionic cadmium in the Wistar rat.离子镉对Wistar大鼠的致畸性。
Arch Toxicol. 1987 Apr;59(6):443-7. doi: 10.1007/BF00316212.
8
The teratogenicity of cadmium-metallothionein in the rat.大鼠中镉-金属硫蛋白的致畸性。
Arch Toxicol. 1988;61(6):457-67. doi: 10.1007/BF00293692.
9
Cadmium effects and biochemical status in hamsters following acute exposure in late gestation.妊娠后期急性暴露后仓鼠体内镉的影响及生化状态
Experientia. 1989 Aug 15;45(8):767-70. doi: 10.1007/BF01974584.