马螺形体病治疗方案:对经乳糖13c -脲醛呼气试验测定的口腔运输时间的特殊影响。

J Kutscha, D G M Sutton, T Preston, A J Guthrie
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引用次数: 6

摘要

进行研究的原因:吡虫威二丙酸是马螺形体病的首选药物,但其服用会引起严重的绞痛和腹泻。需要一种能减少这些影响的吡虫威方案。目的:1)定量测定二丙酸咪唑威在有或没有阿托品或甘罗酸酯预用药的情况下对马口腔运输时间(OCTT)的影响;2)研究咪唑威给药的改进前处理方案。假设:使用二丙酸咪唑威治疗将导致绞痛和降低OCTT,如乳糖13c -脲醛呼气试验所示,这将通过使用阿托品或甘罗酸盐进行预用药来改善。方法:在一项随机双盲研究中,比较3种药物治疗对6匹健康马OCTT的影响与生理盐水对照:1)二丙酸咪唑威2.4 mg/kg bwt肌肉注射(i.m),生理盐水静脉注射(i.v);imidocarb /生理盐水);2)二丙酸咪唑威2.4 mg/kg BWT ig,阿托品0.035 mg/kg BWT ig(咪唑威/阿托品);3)二丙酸咪唑威2.4 mg/kg BWT ig,吡唑威/ glycopyrolate 0.0025 mg/kg BWT ig(咪唑威/ glycopyrolate)。采用乳糖13c -脲醛呼气试验测量每个病例的OCTT,并通过线性模型方差分析确定治疗效果的显著性。结果:吡虫威/阿托品治疗引起OCTT升高(P < 0.05),而吡虫威/生理盐水治疗引起OCTT无显著降低。吡虫威/生理盐水导致6匹马中的4匹马出现绞痛和腹泻,而使用吡虫威/阿托品或吡虫威/甘磺罗酯或使用生理盐水对照的马没有出现这种情况。吡虫威/盐水组马肠道borborgmi增加,吡虫威/阿托品组马肠道borborgmi减少。结论:与吡虫威/生理盐水治疗相比,吡虫威/阿托品治疗显著增加了OCTT,而吡虫威/生理盐水治疗诱导了绞痛症状和潜在的OCTT降低。阿托品和甘替罗酸预用药均能改善吡虫威的临床胃肠道作用,但阿托品对胃和/或小肠运动的抑制作用显著,而甘替罗酸未检测到。当使用吡虫威治疗马螺形体病时,建议预先使用甘罗酸酯。
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Equine piroplasmosis treatment protocols: specific effect on orocaecal transit time as measured by the lactose 13C-ureide breath test.

Reasons for performing study: Imidocarb dipropionate is the drug of choice for equine piroplasmosis but its administration causes severe colic and diarrhoea. An imidocarb protocol that reduces these effects is needed.

Objectives: 1) Quantification of the effects of imidocarb dipropionate on equine orocaecal transit time (OCTT), with and without atropine or glycopyrrolate premedication and 2) investigation of an improved pretreatment regimen for imidocarb administration.

Hypothesis: Treatment with imidocarb dipropionate will result in colic and reduced OCTT as demonstrated by the lactose 13C-ureide breath test which will be ameliorated by premedication with either atropine or glycopyrrolate.

Methods: The effects of 3 drug therapies on OCTT were compared in 6 healthy horses in a randomised double-blind study vs. a saline control: 1) imidocarb dipropionate 2.4 mg/kg bwt administered intramuscularly (i.m.) with saline administered intravenously (i.v.; imidocarb/saline); 2) imidocarb dipropionate 2.4 mg/kg bwt administered i.m. with atropine 0.035 mg/kg bwt administered i.v. (imidocarb/atropine) and 3) imidocarb dipropionate 2.4 mg/kg bwt administered i.m. with glycopyrrolate 0.0025 mg/kg bwt administered i.v. (imidocarb/glycopyrrolate). The lactose 13C-ureide breath test was used to measure OCTT in each case and significance of treatment effect determined by a linear model analysis of variance.

Results: Imidocarb/atropine treatment caused an increase in OCTT (P < 0.05) whereas imidocarb/saline produced a nonsignificant decrease in OCTT. Imidocarb/saline caused colic and diarrhoea in 4 of 6 horses, which were not seen in any of the horses treated with imidocarb/atropine or imidocarb/glycopyrrolate or administered the saline control. Intestinal borborygmi were increased in imidocarb/saline and decreased in imidocarb/atropine treated horses, respectively.

Conclusions: Imidocarb/saline treatment induced colic signs and a potential reduction in OCTT while imidocarb/atropine treatment increased OCTT significantly when compared with imidocarb/saline. Both atropine and glycopyrrolate premedication ameliorated the clinical gastrointestinal effects of imidocarb but atropine produced significant inhibition of gastric and/or small intestinal motility not detected with glycopyrrolate. Premedication with glycopyrrolate is recommended when using imidocarb for treatment of equine piroplasmosis.

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