Retrospective evaluation of combined mycophenolate mofetil and prednisone treatment for meningoencephalomyelitis of unknown etiology in dogs: 25 cases (2005-2011).

Itai Barnoon, Merav H Shamir, Itamar Aroch, Tali Bdolah-Abram, Itai Srugo, Lilach Konstantin, Orit Chai
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引用次数: 33

Abstract

Objective: To evaluate the use of a combined protocol of prednisone and mycophenolate mofetil (MMF) for the treatment of meningoencephalomyelitis of unknown etiology (MUE) and to describe response, adverse effects, and outcome.

Design: Retrospective study (2005-2011).

Setting: University teaching hospital.

Animals: Twenty-five client-owned dogs with clinical signs, neuroimaging, and cerebrospinal abnormalities consistent with MUE. Five dogs whose MMF treatment was discontinued after 7-14 days due to gastrointestinal clinical signs were evaluated only for adverse effects.

Interventions: Dogs were initially treated with prednisone 2 mg/kg PO every 12 hours and with MMF 20 mg/kg PO or IV every 12 hours. Prednisone was tapered after 4 days to 1 mg/kg every 12 hours for 14 days, then to every 24 hours for 30 days, and again reduced by half every 2-4 months thereafter. When prednisone was tapered completely or to 0.5 mg/kg every 24-48 hours without clinical relapse, MMF was tapered in a similar manner.

Measurements and main results: Partial or complete clinical response was achieved in 95% (19/20) of the dogs. Median survival time by the end of the study was 250 days (range 6 to >1,679) with 40% (8/20) of the dogs still alive (336-1,679 days after diagnosis). All Pug dogs (4/20) included in the study died with a median survival time of 14 days. Adverse effects attributed to MMF, which included hemorrhagic diarrhea within the first 2 weeks of treatment, were recorded in 20% (5/25) of the dogs.

Conclusions: MMF can be used as an adjunctive treatment for dogs with MUE. This protocol enables reduction of prednisone treatment or, in some cases, its complete withdrawal. The possibility of intravenous administration is advantageous in cases with severe neurological abnormalities and mentation changes, often seen in MUE. Attention is warranted for gastrointestinal adverse effects, especially in the first 2 weeks of treatment.

霉酚酸酯联合强的松治疗犬不明原因脑膜脊髓炎25例回顾性分析(2005-2011)。
目的:评估强的松和霉酚酸酯(MMF)联合治疗不明原因脑膜脊髓炎(MUE)的应用,并描述反应、不良反应和结局。设计:回顾性研究(2005-2011)。单位:大学教学医院。动物:25只客户拥有的狗,临床症状,神经影像学和脑脊液异常与MUE一致。5只因胃肠道临床症状在7-14天后停止MMF治疗的狗只评估其不良反应。干预措施:最初每12小时给予强的松2 mg/kg PO,每12小时给予MMF 20 mg/kg PO或静脉注射。泼尼松在4天后逐渐减少至每12小时1 mg/kg,持续14天,然后每24小时1 mg/kg,持续30天,之后每2-4个月再次减少一半。当泼尼松完全减少或每24-48小时减少0.5 mg/kg而无临床复发时,MMF也以类似的方式减少。测量和主要结果:95%(19/20)的狗达到部分或完全临床缓解。研究结束时的中位生存时间为250天(范围6至> 1679天),其中40%(8/20)的狗仍然存活(诊断后336- 1679天)。研究中包括的所有巴哥犬(4/20)死亡,平均生存时间为14天。20%(5/25)的狗记录了MMF引起的不良反应,包括治疗前2周的出血性腹泻。结论:MMF可作为MUE犬的辅助治疗。该方案可减少强的松治疗,或在某些情况下完全停药。静脉给药的可能性是有利的情况下,严重的神经异常和精神状态的改变,常见于MUE。需要注意胃肠道不良反应,特别是在治疗的前2周。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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