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胆钙化醇

Cholecalciferol.

作者信息

Peterson Michael E, Fluegeman Kerstin

机构信息

Reid Veterinary Hospital, Albany, OR, USA.

出版信息

Top Companion Anim Med. 2013 Feb;28(1):24-7. doi: 10.1053/j.tcam.2013.03.006.

Abstract

The primary source of exposure to cholecalciferol in dogs and cats is ingestion of rodenticide baits with vitamin D3 as the active ingredient. Other sources of this toxin are human medications and rarely, contaminated pet food. Although the reported lethal dose 50% for cholecalciferol is 88 mg/kg, deaths have been seen with an individual exposure of 2 mc g/kg in dogs. Clinical signs are induced by profound hypercalcemia affecting multiple body systems. Clinical presentations may include anorexia, depression, muscle weakness, vomiting, polyuria, polydipsia, dehydration, abdominal pain, hematemesis, melena, and bradycardia. Tissue mineralization may develop if calcium × phosphorous product is greater than 60. Serum testing for hypercalcemia, hyperphosphatemia, and decreased serum parathyroid hormone are confirmatory. Initial treatment relies upon decontamination with emesis induction followed by administration of pulse-dose activated charcoal designed to interfere with the extensive enterohepatic recirculation of toxin. Medical management is designed to decrease serum calcium levels by use of intravenous fluid diuresis with administration of furosemide and prednisolone. Biphosphate pamidronate is used to inhibit calcium release from the bone. Phosphate binders aid in decreasing phosphate availability to interact with calcium. The prognosis is better if treatment is instituted early before development of hypercalcemia and hyperphosphatemia enables tissue mineralization to progress.

摘要

犬猫接触胆钙化醇的主要来源是摄入以维生素D3为活性成分的灭鼠药饵。这种毒素的其他来源是人类药物,很少见的是受污染的宠物食品。尽管报道的胆钙化醇半数致死剂量为88毫克/千克,但犬单次接触2微克/千克就出现了死亡病例。临床症状是由影响多个身体系统的严重高钙血症引起的。临床表现可能包括厌食、抑郁、肌肉无力、呕吐、多尿、多饮、脱水、腹痛、呕血、黑便和心动过缓。如果钙×磷乘积大于60,可能会发生组织矿化。血清高钙血症、高磷血症检测以及血清甲状旁腺激素降低可作为确诊依据。初始治疗依赖于催吐进行去污,随后给予脉冲剂量活性炭,以干扰毒素广泛的肠肝循环。药物治疗旨在通过静脉补液利尿并给予呋塞米和泼尼松龙来降低血清钙水平。双膦酸盐帕米膦酸用于抑制骨钙释放。磷酸盐结合剂有助于减少磷酸盐与钙相互作用的可能性。如果在高钙血症和高磷血症导致组织矿化进展之前尽早开始治疗,预后会更好。

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