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单异戊酯中-2,3-二巯基丁二酸对急性镉中毒病理学的影响。

Effect of monoisoamyl meso-2,3-dimercaptosuccinate on the pathology of acute cadmium intoxication.

作者信息

Xu C, Holscher M A, Jones M M, Singh P K

机构信息

Department of Chemistry and Center in Molecular Toxicology, Vanderbilt University, Nashville, Tennessee 87235, USA.

出版信息

J Toxicol Environ Health. 1995 Jul;45(3):261-77. doi: 10.1080/15287399509531995.

Abstract

The ability of monoisoamyl meso-2,3-dimercaptosuccinate (Mi-ADMS) to offset the characteristic organ pathology of intraperitoneally administered cadmium chloride (CdCl2) and that of the cadmium-cysteine complex has been examined in male Wistar rats. The tissues examined for damage were the testes, kidney, liver, pancreas, and bone marrow. At a high dose of CdCl2 (0.03 mmol/kg, ip) testicular damage was completely prevented by Mi-ADMS (0.50 mmol/kg, ip) given immediately. A decrease in the protective ability of the antagonist was observed following delayed administration of Mi-ADMS given at 1, 2, 4, and 24 h post CdCl2. At a lower dose of CdCl2 (0.006 mmol/kg, ip), Mi-ADMS furnished essentially full protection from testicular damage when given (0.50 mmol/kg, sc) at 0 and 1 h after CdCl2. The administration of cadmium-cysteine complex (0.01 mmol/kg, ip) induced notable renal tubular damage, which was antagonized by the administration of Mi-ADMS (0.50 mmol/kg, ip) as late as 4 h after the complex. At a 24-h delay, extensive tubular necrosis was found on sacrifice after 4 d. The administration of cadmium-cysteine complex ip reduced, but did not eliminate, the characteristic damage of the seminiferous tubules found for cadmium alone. There is a progressive reduction of testicular weight as the interval between cadmium and antagonist administration increases. The average kidney weights of the animals given CdCl2-cysteine complex were increased in comparison to normal controls. The antagonistic effects of Mi-ADMS treatment on cadmium intoxication in the kidneys and the testes of rats is very similar to that found for effective dithiocarbamate antagonists. In order to obtain complete protection of the testes from the deteterious effects of cadmium, such antagonists must be administered no later than about 1 h after the cadmium.

摘要

在雄性Wistar大鼠中,研究了单异戊酯内消旋-2,3-二巯基琥珀酸(Mi-ADMS)抵消腹腔注射氯化镉(CdCl2)及镉-半胱氨酸复合物所致特征性器官病变的能力。检测受损的组织有睾丸、肾脏、肝脏、胰腺和骨髓。在高剂量CdCl2(0.03 mmol/kg,腹腔注射)时,立即给予Mi-ADMS(0.50 mmol/kg,腹腔注射)可完全预防睾丸损伤。在CdCl2注射后1、2、4和24小时给予Mi-ADMS,延迟给药后观察到拮抗剂的保护能力下降。在较低剂量CdCl2(0.006 mmol/kg,腹腔注射)时,在CdCl2后0和1小时给予Mi-ADMS(0.50 mmol/kg,皮下注射)可基本完全保护免受睾丸损伤。腹腔注射镉-半胱氨酸复合物(0.01 mmol/kg)可引起明显的肾小管损伤,在复合物注射后4小时给予Mi-ADMS(0.50 mmol/kg,腹腔注射)可拮抗这种损伤。延迟24小时后,处死4天后发现广泛的肾小管坏死。腹腔注射镉-半胱氨酸复合物可减轻但不能消除单独镉所致的生精小管特征性损伤。随着镉与拮抗剂给药间隔时间的增加,睾丸重量逐渐减轻。与正常对照组相比,给予CdCl2-半胱氨酸复合物的动物平均肾脏重量增加。Mi-ADMS治疗对大鼠肾脏和睾丸镉中毒的拮抗作用与有效的二硫代氨基甲酸盐拮抗剂非常相似。为了使睾丸完全免受镉的有害影响,此类拮抗剂必须在镉注射后不迟于约1小时给药。

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