ECO Animal Health Ltd, London, UK.
Moredun Scientific Ltd, Pentlands Science Park, Bush Loan, Penicuik, Midlothian, EH26 0PZ, UK.
BMC Vet Res. 2023 Feb 1;19(1):31. doi: 10.1186/s12917-023-03571-x.
The effect of a water-soluble formulation of tylvalosin (Aivlosin® 625 mg/g granules) on disease caused by porcine reproductive and respiratory syndrome virus (PRRSV) and Mycoplasma hyopneumoniae (Mhyop) was investigated in two animal studies. In a PRRSV challenge model in pregnant sows (n = 18), six sows received water medicated at target dose of 5 mg tylvalosin/kg body weight/day from 3 days prior to challenge until the end of gestation. Six sows were left untreated, with a third group remaining untreated and unchallenged. Sows were challenged with PRRSV-2 at approximately 85 days of gestation. Cytokines, viremia, viral shedding, sow reproductive parameters and piglet performance to weaning were evaluated. In a dual infection study (n = 16), piglets were challenged with Mhyop on days 0, 1 and 2, and with PRRSV-1 on day 14 and euthanized on day 24. From day 10 to 20, eight piglets received water medicated at target dose of 20 mg tylvalosin/kg body weight/day and eight piglets were left untreated. Cytokines, viremia, bacteriology and lung lesions were evaluated.
In the PRRSV challenge study in pregnant sows, tylvalosin significantly reduced the levels of serum IL-8 (P < 0.001), IL-12 (P = 0.032), TNFα (P < 0.001) and GM-CSF (P = 0.001). IL-8 (P = 0.100) tended to be lower in uterus of tylvalosin sows. All piglets from tylvalosin sows surviving to weaning were PRRSV negative in faecal swabs at weaning compared to 33.3% PRRSV positive piglets from untreated sows (P = 0.08). In the dual challenge study in piglet, tylvalosin reduced serum IL1β, IL-4, IL-6, IL-8, IL-10, IL-12, IL-1α, IL-13, IL-17A, IL-18, GM-CSF, TGFβ1, TNFα, CCL3L1, MIG, PEPCAM-1 (P < 0.001) and increased serum IFNα, IL-1ra and MIP-1b (P < 0.001). In the lungs, tylvalosin reduced IL-8, IL-10 and IL-12 compared to untreated pigs (P < 0.001) and tended to reduce TNFα (P = 0.082). Lung lavage samples from all tylvalosin treated piglets were negative for Mhyop (0 cfu/mL) compared to the untreated piglets which had mean Mhyop counts of 2.68 × 10 cfu/mL (P = 0.023).
Overall, tylvalosin reduced both local and systemic proinflammatory cytokines after challenge with respiratory pathogens in sows and in piglets. Tylvalosin was effective in reducing Mhyop recovery from the lungs and may reduce virus shedding in piglets following transplacental PRRSV infection in sows.
在两项动物研究中,考察了水溶性替米考星制剂(Aivlosin® 625mg/g 颗粒)对猪繁殖与呼吸综合征病毒(PRRSV)和猪肺炎支原体(Mhyop)引起的疾病的影响。在妊娠母猪的 PRRSV 攻毒模型中(n=18),6 头母猪从攻毒前 3 天开始至妊娠结束时,以 5mg 替米考星/公斤体重/天的目标剂量接受饮水给药。6 头母猪未接受治疗,第三组母猪既未接受治疗也未受到攻毒。母猪在妊娠约 85 天时接受 PRRSV-2 攻毒。评估了细胞因子、病毒血症、病毒脱落、母猪繁殖参数和仔猪断奶性能。在双重感染研究中(n=16),猪在 0、1 和 2 日龄时接受 Mhyop 攻毒,在 14 日龄时接受 PRRSV-1 攻毒,并在 24 日龄时安乐死。从第 10 天到第 20 天,8 头仔猪接受以 20mg 替米考星/公斤体重/天的目标剂量饮水给药,8 头仔猪未接受治疗。评估了细胞因子、病毒血症、细菌学和肺脏病变。
在妊娠母猪的 PRRSV 攻毒研究中,替米考星显著降低了血清中 IL-8(P<0.001)、IL-12(P=0.032)、TNFα(P<0.001)和 GM-CSF(P=0.001)的水平。子宫中 IL-8(P=0.100)在替米考星母猪中趋于较低水平。所有存活至断奶的替米考星母猪的仔猪在断奶时粪便拭子中 PRRSV 均为阴性,而未接受治疗的母猪的仔猪中 33.3%为 PRRSV 阳性(P=0.08)。在仔猪的双重攻毒研究中,替米考星降低了血清中 IL1β、IL-4、IL-6、IL-8、IL-10、IL-12、IL-1α、IL-13、IL-17A、IL-18、GM-CSF、TGFβ1、TNFα、CCL3L1、MIG、PEPCAM-1(P<0.001),并增加了血清 IFNα、IL-1ra 和 MIP-1b(P<0.001)。在肺部,替米考星降低了与未接受治疗的猪相比,IL-8、IL-10 和 IL-12 的水平(P<0.001),且 IL-12 水平有降低趋势(P=0.082)。所有接受替米考星治疗的仔猪的肺灌洗液样本中均未检测到 Mhyop(0cfu/mL),而未接受治疗的仔猪 Mhyop 计数平均值为 2.68×10cfu/mL(P=0.023)。
总体而言,替米考星在母猪和仔猪中经呼吸道病原体攻毒后,降低了局部和全身促炎细胞因子。替米考星在降低 Mhyop 从肺部恢复方面有效,并可能降低母猪经胎盘 PRRSV 感染后仔猪的病毒脱落。
