Clinic of Medicine, Faculty of Veterinary Science, University of Thessaly, 224 Trikalon Str., GR-43132, Karditsa, Greece; Veterinary Clinic "St. Modestos", Aerodromiou Str. 59A, GR-57013, Thessaloniki, Greece.
Clinic of Medicine, Faculty of Veterinary Science, University of Thessaly, 224 Trikalon Str., GR-43132, Karditsa, Greece.
Exp Parasitol. 2020 Jul;214:107903. doi: 10.1016/j.exppara.2020.107903. Epub 2020 Apr 28.
The aim of this 6-month, randomized, blinded, controlled clinical trial was to compare the efficacy and safety of aminosidine-allopurinol combination with that of meglumine antimoniate-allopurinol combination for the treatment of leishmaniosis in dogs without stage III or IV chronic kidney disease. Forty client-owned dogs were randomly assigned to group A [n = 20; aminosidine (15 mg/kg, subcutaneously, once daily, for 28 days) and allopurinol (10 mg/kg, per os, twice daily, for 6 months)] or group B [(n = 20; meglumine antimoniate (100 mg/kg SC, once daily, for 28 days) and allopurinol (10 mg/kg, per os, twice daily, for 6 months)]. Clinical and clinicopathological evaluations, parasitic load measurement (lymph node and bone marrow microscopy, bone marrow real-time PCR), specific serology and leishmanin skin test (LST) were performed at baseline (time 1) and after 14 (time 2), 28 (time 3), 60 (time 4) and 180 (time 5) days. Both treatments were safe and resulted in significant clinical and clinicopathological improvement, reduction of parasitic load and of indirect immunofluorescence antibody test (IFAT) titer and induction of positive LST. There was no significant difference between groups with regards to the primary outcome measures of the trial that included the proportion of dogs that presented severe treatment-related side effects, were cured and were parasitologically negative at time 5. However, some (proportion of dogs that presented no clinical signs, no hyperglobulinemia and negative serology at time 5) secondary outcome measures showed significant differences in favor of the meglumine antimoniate-allopurinol treatment arm. Treatment-related death occurred in one dog in each group, while injection site reactions appeared at a similar frequency in both groups. Due to the differences in some secondary outcome measures in association with the low power of this trial, it cannot be definitively concluded that the two treatments are equally effective. Therefore, the aminisodine-allopurinol combination cannot be proposed as a first-line treatment of CanL but rather as a second-line treatment that may be particularly useful to avoid repeated administration of meglumine antimoniate and in countries where the latter is not available or registered.
本为期 6 个月、随机、双盲、对照的临床试验旨在比较阿米诺霉素-别嘌醇联合疗法与葡甲胺锑-别嘌醇联合疗法治疗无 III 或 IV 期慢性肾病犬利什曼病的疗效和安全性。将 40 只患犬随机分配至 A 组(n=20;阿米诺霉素(15mg/kg,皮下注射,每日 1 次,连用 28 天)和别嘌醇(10mg/kg,口服,每日 2 次,连用 6 个月))或 B 组(n=20;葡甲胺锑(100mg/kg,皮下注射,每日 1 次,连用 28 天)和别嘌醇(10mg/kg,口服,每日 2 次,连用 6 个月))。在基线(时间 1)以及 14 天(时间 2)、28 天(时间 3)、60 天(时间 4)和 180 天(时间 5)时进行临床和临床病理评估、寄生虫载量测量(淋巴结和骨髓显微镜检查、骨髓实时 PCR)、特异性血清学和利什曼素皮肤试验(LST)。两种治疗均安全有效,可显著改善临床和临床病理,降低寄生虫载量和间接免疫荧光抗体试验(IFAT)滴度,并诱导阳性 LST。在试验的主要结局指标(包括出现严重治疗相关副作用、治愈和 5 天时寄生虫学阴性的犬比例)方面,两组间无显著差异。然而,一些(5 天时无临床症状、无高球蛋白血症和阴性血清学的犬比例)次要结局指标显示出有利于葡甲胺锑-别嘌醇治疗组的显著差异。每组各有 1 只犬因治疗相关死亡,而两组的注射部位反应发生率相似。由于一些次要结局指标的差异以及本试验的效能较低,不能确定两种治疗方法的疗效完全相同。因此,阿米诺霉素-别嘌醇联合疗法不能作为犬利什曼病的一线治疗方法,而更适用于避免重复使用葡甲胺锑,且在后者不可用或未注册的国家。
