Department of Animal Science, Iowa State University, Ames, IA 50011.
Department of Veterinary Microbiology and Preventive Medicine, Iowa State University, Ames, IA 50011.
J Dairy Sci. 2024 Aug;107(8):6225-6239. doi: 10.3168/jds.2023-24350. Epub 2024 Feb 29.
Cows in early lactation (EL) are purportedly immune suppressed, which renders them more susceptible to disease. Thus, the study objective was to compare key biomarkers of immune activation from i.v. LPS between EL and mid-lactation (ML) cows. Multiparous EL (20 ± 2 DIM; n = 11) and ML (131 ± 31 DIM; n = 12) cows were enrolled in a 2 × 2 factorial design and assigned to 1 of 2 treatments by lactation stage (LS): (1) EL (EL-LPS; n = 6) or ML (ML-LPS; n = 6) cows administered a single LPS bolus from Escherichia coli O55:B5 (0.09 µg/kg of BW), or (2) pair-fed (PF) EL (EL-PF; n = 5) or ML (ML-PF; n = 6) cows administered i.v. saline. After LPS administration, cows were intensely evaluated for 3 d to analyze their response and recovery to LPS. Rectal temperature increased in LPS relative to PF cows (1.1°C in the first 9 h), and the response was more severe in EL-LPS relative to ML-LPS cows (2.3 vs. 1.3°C increase at 4 h post-LPS; respectively). Respiration rate increased only in EL-LPS cows (47% relative to ML-LPS in the first hour post-LPS). Circulating tumor necrosis factor-α, IL-6, monocyte chemoattractant protein-1, macrophage inflammatory protein (MIP)-1α, MIP-1β, and IFN-γ-inducible protein-10 increased within the first 6 h after LPS and these changes were exacerbated in EL-LPS relative to ML-LPS cows (6.3-fold, 4.8-fold, 57%, 93%, 10%, and 61%, respectively). All cows administered LPS had decreased circulating iCa relative to PF cows (34% at the 6 h nadir), but the hypocalcemia was more severe in EL-LPS than ML-LPS cows (14% at 6 h nadir). In response to LPS, neutrophils decreased regardless of LS, then increased into neutrophilia by 24 h in all LPS relative to PF cows (2-fold); however, the neutrophilic phase was augmented in EL- compared with ML-LPS cows (63% from 24 to 72 h). Lymphocytes and monocytes rapidly decreased then gradually returned to baseline in LPS cows regardless of LS; however, monocytes were increased (57%) at 72 h in EL-LPS relative to ML-LPS cows. Platelets were reduced (46%) in LPS relative to PF cows throughout the 3-d following LPS, and from 24 to 48 h, platelets were further decreased (41%) in EL-LPS compared with ML-LPS. During the 3-d following LPS, serum amyloid A (SAA), LPS-binding protein (LBP), and haptoglobin (Hp) increased in LPS compared with PF groups (9-fold, 72%, and 153-fold, respectively), and the LBP and Hp responses were more exaggerated in EL-LPS than ML-LPS cows (85 and 79%, respectively) whereas the SAA response did not differ by LS. Thus, our data indicates that EL immune function does not appear "suppressed," and in fact many aspects of the immune response are seemingly functionally robust.
奶牛在泌乳早期(EL)据称存在免疫抑制,这使它们更容易患病。因此,本研究的目的是比较来自静脉内 LPS 的 EL 和泌乳中期(ML)奶牛的免疫激活的关键生物标志物。多胎 EL(20 ± 2 DIM;n = 11)和 ML(131 ± 31 DIM;n = 12)奶牛按泌乳阶段(LS)参与了 2 × 2 析因设计,并被分配到 2 种处理之一:(1)EL(EL-LPS;n = 6)或 ML(ML-LPS;n = 6)奶牛接受大肠杆菌 O55:B5(0.09 µg/kg BW)的单次 LPS 冲击,或(2)等量喂养(PF)EL(EL-PF;n = 5)或 ML(ML-PF;n = 6)奶牛接受静脉内盐水。在 LPS 给药后,对奶牛进行了 3 天的密集评估,以分析它们对 LPS 的反应和恢复情况。与 PF 奶牛相比,LPS 给药后直肠温度升高(前 9 小时升高 1.1°C),EL-LPS 奶牛的反应比 ML-LPS 奶牛更严重(4 小时时分别增加 2.3°C 和 1.3°C)。只有 EL-LPS 奶牛的呼吸频率增加(LPS 后第 1 小时增加 47%)。循环肿瘤坏死因子-α、IL-6、单核细胞趋化蛋白-1、巨噬细胞炎性蛋白(MIP)-1α、MIP-1β 和 IFN-γ 诱导蛋白-10 在 LPS 后前 6 小时内增加,这些变化在 EL-LPS 奶牛中加剧(分别为 6.3 倍、4.8 倍、57%、93%、10%和 61%)。与 PF 奶牛相比,所有接受 LPS 的奶牛的循环 iCa 均降低(6 小时时最低值为 34%),但 EL-LPS 奶牛的低钙血症比 ML-LPS 奶牛更严重(6 小时时最低值为 14%)。对 LPS 作出反应后,无论 LS 如何,中性粒细胞均减少,然后在所有 LPS 奶牛中在 24 小时内增加到中性粒细胞增多(2 倍);然而,EL 中的中性粒细胞相增强与 ML-LPS 奶牛相比(63%,从 24 小时到 72 小时)。无论 LS 如何,LPS 奶牛的淋巴细胞和单核细胞迅速减少,然后逐渐恢复到基线;然而,与 ML-LPS 奶牛相比,EL-LPS 奶牛在 72 小时时单核细胞增加(57%)。与 PF 奶牛相比,LPS 奶牛在 LPS 后 3 天内的血小板减少(46%),从 24 小时到 48 小时,EL-LPS 奶牛的血小板进一步减少(41%)。在 LPS 后 3 天内,血清淀粉样蛋白 A(SAA)、LPS 结合蛋白(LBP)和触珠蛋白(Hp)在 LPS 组中比 PF 组增加(分别增加 9 倍、72%和 153 倍),LBP 和 Hp 的反应在 EL-LPS 奶牛中比 ML-LPS 奶牛更明显(分别为 85%和 79%),而 SAA 反应不受 LS 影响。因此,我们的数据表明,EL 免疫功能似乎没有“受到抑制”,事实上,免疫反应的许多方面似乎具有强大的功能。
