低体细胞计数奶牛泌乳期末单独使用乳头内封闭剂引起临床或亚临床乳腺炎的风险因素。
Risk factors for clinical or subclinical mastitis following infusion of internal teat sealant alone at the end of lactation in cows with low somatic cell counts.
机构信息
Cognosco, Anexa, Morrinsville, New Zealand.
DairyNZ Ltd, Hamilton, New Zealand.
出版信息
N Z Vet J. 2022 Mar;70(2):79-87. doi: 10.1080/00480169.2021.1977200. Epub 2021 Oct 3.
AIMS
To identify risk factors for subclinical and clinical mastitis in cows with low somatic cell counts (SCC) following infusion with internal teat sealant (ITS) at drying off.
METHODS
Cows with no history of clinical mastitis and a maximum SCC <250,000 cells/mL at any herd test in the lactation before drying off were randomly selected from 36 herds. In the final week of lactation, quarter milk samples were collected aseptically from each selected cow for microbiology, and each quarter was then infused with ITS. Clinical mastitis records from 22 herds and herd test data from all herds were collated to determine potential herd- or cow-level explanatory variables for clinical mastitis over the dry period or in the first 60 days of the subsequent lactation, and subclinical mastitis (SCC >200,000 cells/mL; SCM) at the first herd test after calving. Multivariable, multilevel, logistic regression analyses were used to model the data.
RESULTS
At drying off, 44/1,514 (2.8%) cows were infected with a major pathogen. Two of 1,001 (0.2%) cows were diagnosed with clinical mastitis over the dry period. There were 128/1,514 (8.5%) cows with SCM at the first herd test after calving. The odds of SCM were greater for cows with a major pathogen present at drying off than those without (OR = 4.7 (95% CI = 2.29-9.65); p < 0.001), and for third or greater lactation than second lactation cows (OR = 3.16 (95% CI = 1.70-5.88); p < 0.001). For every 1L increase in milk yield at the last herd test before drying off the OR for SCM was 1.07 (95% CI = 1.01-1.13); (p = 0.02), and for each 1 unit increase in ln maximum SCC in the lactation before drying off the OR for SCM was 1.54 (95% CI = 1.13-2.10); (p = 0.01). There were 30/976 (3.1%) cows diagnosed with clinical mastitis in the first 60 days after calving. The odds of clinical mastitis were greater for cows producing >15 L/day at the last herd test of the preceding lactation than cows producing <10 L/day (OR = 4.79 (95% CI = 1.48-15.46); p = 0.009); for each 1 unit increase in ln maximum SCC in the previous lactation the OR for clinical mastitis was 1.96 (95% CI = 1.09-3.54); (p = 0.03), and the odds increased with increasing herd-level cow-case lactational incidence of clinical mastitis in the preceding lactation (p = 0.003).
CONCLUSIONS AND CLINICAL RELEVANCE
Selection of cows with low SCC for ITS infusion should consider cow milk yield and maximum cow SCC in the preceding lactation.
目的
确定在干奶期内使用内部乳头密封剂(ITS)后,体细胞计数(SCC)较低的奶牛发生亚临床和临床乳腺炎的风险因素。
方法
从 36 个牛群中随机选择在干奶前的泌乳期内任何一次群体检测中没有临床乳腺炎病史且最大 SCC<250000 个细胞/ml 的奶牛。在泌乳期末的最后一周,无菌采集每头选定奶牛的四分奶样进行微生物学检测,然后对每个四分奶样进行 ITS 灌注。整理来自 22 个牛群的临床乳腺炎记录和来自所有牛群的群体检测数据,以确定干奶期或随后泌乳期的头/牛水平上的潜在乳腺炎解释变量,以及产后第一次群体检测时的亚临床乳腺炎(SCC>200000 个细胞/ml;SCM)。使用多变量、多层次逻辑回归分析来对数据进行建模。
结果
在干奶期,44/1514(2.8%)头奶牛感染了主要病原体。1001 头奶牛中有 2 头(0.2%)在干奶期内被诊断为临床乳腺炎。产后第一次群体检测时,有 128/1514(8.5%)头奶牛发生 SCM。与没有主要病原体的奶牛相比,在干奶期存在主要病原体的奶牛发生 SCM 的几率更高(OR=4.7(95%CI=2.29-9.65);p<0.001),与第二泌乳期的奶牛相比,第三次或以上泌乳期的奶牛发生 SCM 的几率更高(OR=3.16(95%CI=1.70-5.88);p<0.001)。在干奶前的最后一次群体检测中,牛奶产量每增加 1L,SCM 的发生几率就会增加 1.07(95%CI=1.01-1.13);(p=0.02),在干奶前的泌乳期内,最大 SCC 的自然对数每增加 1 个单位,SCM 的发生几率就会增加 1.54(95%CI=1.13-2.10);(p=0.01)。在产后的头 60 天内,有 30/976(3.1%)头奶牛被诊断为临床乳腺炎。与产奶量<10L/d 的奶牛相比,在上一个泌乳期的最后一次群体检测中,产奶量>15L/d 的奶牛发生临床乳腺炎的几率更高(OR=4.79(95%CI=1.48-15.46);p=0.009);与上一个泌乳期的最大 SCC 的自然对数每增加 1 个单位相比,临床乳腺炎的发生几率增加 1.96(95%CI=1.09-3.54);(p=0.03),并且随着上一个泌乳期中群体水平的奶牛乳腺炎病例发病率的增加,临床乳腺炎的几率也会增加(p=0.003)。
结论和临床意义
为 ITS 灌注选择 SCC 较低的奶牛时,应考虑奶牛的产奶量和上一个泌乳期的最大 SCC。
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