Effect of rumen-protected choline on dairy cow metabolism, immunity, lactation performance, and vaginal discharge microbiome

被引:0
|
作者
Marques, T. C. [1 ,2 ]
Monteiro, H. F. [1 ]
Melo, D. B. [1 ]
Coelho, W. M. [1 ]
Salman, S. [1 ]
Marques, L. R. [2 ]
Leao, K. M. [2 ]
Machado, V. S. [3 ]
Menta, P. [3 ]
Dubey, D. [4 ]
Sun, F. [5 ]
Lima, F. S. [1 ]
机构
[1] Univ Calif Davis, Dept Populat Hlth & Reprod, Davis, CA 95616 USA
[2] Inst Fed Goiano, Dept Anim Sci, BR-75901970 Rio Verde, GO, Brazil
[3] Texas Tech Univ, Coll Agr Sci & Nat Resources, Dept Vet Sci, Lubbock, TX 79409 USA
[4] Kemin Europa NV, B-2640 Herentals, Belgium
[5] Kemin Ind Inc, Des Moines, IA 50317 USA
关键词
inflammatory response; energy homeostasis; lipids; microbiome; PREPARTUM ENERGY-INTAKE; TRANSITION PERIOD; BLOOD METABOLITES; SUPPLEMENTATION; REPRODUCTION; GLUCOSE; HAPTOGLOBIN; ASSOCIATION; NEUTROPHIL; METHIONINE;
D O I
10.3168/jds.2023-23850
中图分类号
S8 [畜牧、 动物医学、狩猎、蚕、蜂];
学科分类号
0905 ;
摘要
Rumen-protected choline (RPC) promotes benefits in milk production, immunity, and health in dairy cows by optimizing lipid metabolism during transition period management and early lactation. However, the RPC success in dairy cows depends on choline bioavailability, which is affected by the type of protection used in rumen-protected choline. Therefore, our objectives were to determine the effects of a novel RPC on dry matter intake (DMI), identify markers of metabolism and immunity, and evaluate lactation performance. Dry Holstein (n = 48) cows at 245 +/- 3 d of gestation were blocked by parity and assigned to control or RPC treatment within each block. Cows enrolled in the RPC treatment received 15 g/d of CholiGEM (Kemin Industries, Cavriago RE, Italy) from 21 d prepartum and 30 g/d of CholiGEM from calving to 21 d postpartum. During the transition period, DMI was measured daily, and blood was sampled weekly for energy-related metabolites such as beta-hydroxybutyrate (BHB), glucose, and nonesterified fatty acids (NEFA), as well as immune function markers such as haptoglobin (Hp) and lipopolysaccharide-binding protein (LPB). Vaginal discharge samples were collected at the calving and 7 d postpartum and stored in microcentrifuge tubes at -80 degrees C until 16S rRNA sequencing. The main responses of body condition score, body weight, DMI, milk yield, milk components, and immune function markers were analyzed using the GLIMMIX procedure of SAS with the effects of treatment, time, parity, and relevant covariates added to the models. The relative abundance of microbiome alpha-diversity was evaluated by 3 indexes (Chao1, Shannon, and Simpson) and beta-diversity by principal coordinate analysis and permutational multi- variate ANOVA. We found no differences in DMI in the pre- and postpartum periods. Cows fed RPC increased the yields of energy- and 3.5% fat-corrected milk and fat yield in primiparous and multiparous cows, with an interaction between treatment and parity for these lactation variables. However, we found no differences in milk protein and lactose up to 150 DIM between treatments. Glucose, NEFA, and BHB had no differences between the treatments. However, RPC decreased BHB numerically (control = 1.07 +/- 0.13 vs. RPC = 0.63 +/- 0.13) in multiparous on the third week postpartum and tended to reduce the incidence of subclinical ketosis (12.7% vs. 4.2%). No effects for Hp and LPB were found in cows fed RPC. Chao1, Shannon, and Simpson indexes were lower at calving in the RPC treatment than in the Control. However, no differences were found 7 d later for Chao1, Shannon, and Simpson indexes. The vaginal discharge microbiome was altered in cows fed RPC at 7 d postpartum. Fusobacterium, , a common pathogen associated with metritis, was reduced in cows fed RPC. Rumen-protected choline enhanced lactation performance and health and altered the vaginal discharge microbiome which is a potential proxy for uterine healthy in dairy cows. The current study's findings corroborate that RPC is a tool to support adaptation to lactation and shed light on opportunities for further research in reproductive health.
引用
收藏
页码:2864 / 2882
页数:19
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