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秋水仙碱与酮康唑在中国沙皮犬中的不良相互作用。

Adverse interaction between colchicine and ketoconazole in a Chinese shar pei.

作者信息

McAlister Amber, Center Sharon A, Bender Hannah, McDonough Sean P

机构信息

Sage Veterinary Specialty and Emergency Centers in Campbell, CA (A.M.); Department of Clinical Sciences (S.C., S.M.) and Department of Biomedical Sciences (H.B.), College of Veterinary Medicine, Cornell University, Ithaca, NY.

出版信息

J Am Anim Hosp Assoc. 2014 Nov-Dec;50(6):417-23. doi: 10.5326/JAAHA-MS-6080.

Abstract

A Chinese shar pei with a 2 yr history of episodic fever, lethargy, and shifting lameness was presumptively diagnosed with familial shar pei fever but had never been treated for the syndrome. After being presented for a superficial pyoderma with possible dermatophyte coinfection, treatment with a cephalosporin and ketoconazole were prescribed. One wk later, colchicine was initiated for familial shar pei fever using cautious dose escalation. Nevertheless, gastrointestinal toxicity, skeletal muscle myopathy, and hepatotoxicity developed within 2 wk. Abrupt resolution of gastrointestinal toxicity and myopathy followed drug withdrawal. However, escalating liver enzyme activity and hyperbilirubinemia led to liver biopsy to rule out an antecedent hepatopathy. Biopsy characterized canalicular cholestasis and colchicine-associated metaphase arrest and ring mitoses reflecting repression of mitotic spindle formation. Signs of illness completely resolved 3 mo after drug discontinuation. Although avoidable adverse interactions between ketoconazole and drugs reliant on cytochrome oxidase biotransformation and/or drug efflux mediated by multiple drug-resistant transporters are well documented in humans, these are rarely reported in veterinary patients. This case exemplifies an important and avoidable ketoconazole/colchicine drug interaction from which the patient completely recovered. The dog tested negative for the canine MDR1 loss of function mutation that also might potentiate colchicine toxicity.

摘要

一只患有间歇性发热、嗜睡和转移性跛行2年病史的中国沙皮犬被初步诊断为家族性沙皮犬热,但从未接受过该综合征的治疗。在因可能合并皮肤癣菌感染而出现浅表脓皮病就诊后,开具了头孢菌素和酮康唑进行治疗。1周后,开始使用秋水仙碱治疗家族性沙皮犬热,并谨慎增加剂量。然而,在2周内出现了胃肠道毒性、骨骼肌肌病和肝毒性。停药后,胃肠道毒性和肌病突然缓解。然而,肝酶活性升高和高胆红素血症导致进行肝活检以排除先前存在的肝病。活检显示为胆小管胆汁淤积以及秋水仙碱相关的中期阻滞和环状有丝分裂,反映有丝分裂纺锤体形成受到抑制。停药3个月后,疾病症状完全消失。虽然酮康唑与依赖细胞色素氧化酶生物转化和/或由多种耐药转运蛋白介导的药物外排的药物之间可避免的不良相互作用在人类中有充分记录,但在兽医患者中很少报道。该病例体现了一种重要且可避免的酮康唑/秋水仙碱药物相互作用,患者已完全康复。这只狗检测犬MDR1功能缺失突变呈阴性,该突变也可能增强秋水仙碱的毒性。

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