Investigation of HCAR2 antagonists as a potential strategy to modulate bovine leukocytes.

IF 6.3 Q1 AGRICULTURE, DAIRY & ANIMAL SCIENCE Journal of Animal Science and Biotechnology Pub Date : 2024-03-06 DOI:10.1186/s40104-024-00999-5
Laman K Mamedova, Kirby C Krogstad, Paiton O McDonald, Laxman Pokhrel, Duy H Hua, Evan C Titgemeyer, Barry J Bradford
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Abstract

Background: Dairy cows experiencing ketosis after calving suffer greater disease incidence and are at greater risk of leaving the herd. In vitro administration of beta-hydroxybutyric acid (BHBA; the primary blood ketone) has inhibitory effects on the function of bovine leukocytes. BHBA is a ligand of HCAR2 and the activation of these receptors promotes an anti-inflammatory response which may be related with immunosuppression observed in transition dairy cattle. The objective of this study was to identify and test antagonists for HCAR2 in bovine immune cells cultured with BHBA.

Results: We observed expression of HCAR2 at the protein level within lymphocytes, monocytes, and granulocytes. The proportion of cells expressing HCAR2 tended to be greater in mid-lactation compared to early lactation cows; the increase was a result of increased proportion of T and B cells expressing HCAR2. Stimulation of HCAR2 with niacin or BHBA promoted Ca2+ mobilization in neutrophils and mononuclear cells. Mononuclear cells treated with BHBA had diminished intracellular Ca2+ responses when HCAR2 was knocked down by siRNA silencing, indicating Ca2+ mobilization was mediated by HCAR2 signaling. Two candidate antagonists for HCAR2, synthesized from niacin (NA-1 and NA-5), were tested; monocytes and neutrophils pre-treated with NA-1 and NA-5 had reduced Ca2+ mobilization after incubation with BHBA. Furthermore, NA-5 but not NA-1 prevented BHBA-associated reductions in cyclic AMP.

Conclusions: We demonstrated that HCAR2 is present on bovine leukocytes and has greater expression later in lactation. We confirmed that BHBA and niacin derived HCAR2 antagonists alter bovine leukocyte activity. Our results demonstrate that both BHBA and niacin affect bovine leukocyte Ca2+ mobilization in a HCAR2-dependent manner.

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将 HCAR2 拮抗剂作为调节牛白细胞的潜在策略的研究。
背景:产犊后出现酮病的奶牛发病率更高,离开牛群的风险也更大。体外给药β-羟丁酸(BHBA;主要血酮)对牛白细胞的功能有抑制作用。BHBA 是 HCAR2 的配体,激活这些受体可促进抗炎反应,这可能与过渡期奶牛的免疫抑制有关。本研究的目的是在用 BHBA 培养的牛免疫细胞中鉴定和测试 HCAR2 的拮抗剂:结果:我们在淋巴细胞、单核细胞和粒细胞中观察到蛋白水平的 HCAR2 表达。表达 HCAR2 的细胞比例在泌乳中期往往高于泌乳早期;这是表达 HCAR2 的 T 细胞和 B 细胞比例增加的结果。用烟酸或 BHBA 刺激 HCAR2 可促进中性粒细胞和单核细胞的 Ca2+ 迁移。当通过 siRNA 沉默敲除 HCAR2 时,用 BHBA 处理的单核细胞的细胞内 Ca2+ 反应减弱,这表明 Ca2+ 迁移是由 HCAR2 信号传导介导的。测试了两种由烟酸合成的 HCAR2 候选拮抗剂(NA-1 和 NA-5);经 NA-1 和 NA-5 预处理的单核细胞和中性粒细胞在与 BHBA 培养后,Ca2+ 迁移减少。此外,NA-5 而非 NA-1 能防止 BHBA 导致的环磷酸腺苷减少:结论:我们证明了牛白细胞中存在 HCAR2,而且在泌乳后期其表达量更大。我们证实,BHBA 和烟酸衍生的 HCAR2 拮抗剂会改变牛白细胞的活性。我们的结果表明,BHBA 和烟酸都会以 HCAR2 依赖性方式影响牛白细胞 Ca2+ 的调动。
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CiteScore
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822
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