Department of Animal Science, Cornell University, Ithaca, NY 14853.
Lilly Research Laboratories, Eli Lilly and Company, Indianapolis, IN 46285.
J Dairy Sci. 2019 Dec;102(12):11597-11608. doi: 10.3168/jds.2019-16696. Epub 2019 Sep 20.
Dairy cows cope with severe energy insufficiency in early lactation by engaging in intense and sustained mobilization of fatty acids from adipose tissue. An unwanted side effect of this adaptation is excessive lipid accumulation in the liver, which in turn impairs hepatic functions. Mice experiencing increased hepatic fatty acid flux are protected from this condition through coordinated actions of the newly described hormone fibroblast growth factor-21 (FGF21) on liver and adipose tissue. The possibility of an analogous role for FGF21 in dairy cows is suggested by its rapid increase in plasma levels around parturition followed by chronically elevated levels in the first few weeks of lactation. To test this hypothesis, dairy cows were randomly assigned on d 12.6 ± 2.2 (± standard error) of lactation to receive either an excipient (control; n = 6) or recombinant human FGF21 (n = 7), first as an FGF21 bolus of 3 mg/kg of body weight (BW) followed 2 d later by a constant i.v. infusion of FGF21 at a rate of 6.3 mg/kg of metabolic BW for 9 consecutive days. After bolus administration, human FGF21 circulated with a half-life of 194 min, and its constant infusion increased total plasma concentration 117-fold over levels in excipient-infused cows. The FGF21 treatment had no effect on voluntary feed intake, milk yield, milk energy output, or net energy balance measured over the 9-d infusion or on final BW. Plasma fatty acids circulated at lower concentrations in the FGF21 group than in the control group for the 8-h period following bolus administration, but this reduction was not significant during the period of constant i.v. infusion. Treatment with FGF21 caused a 50% reduction in triglyceride content in liver biopsies taken at the end of the constant i.v. infusion without altering the mRNA abundance of key genes involved in the transport, acyl coenzyme A activation, or oxidation of fatty acids. In contrast, FGF21 treatment ablated the recovery of plasma insulin-like growth factor-1 seen in control cows during the 9-d i.v. infusion period despite a tendency for higher plasma growth hormone. This effect was associated with increased hepatic mRNA abundance of the intracellular inhibitor of growth hormone receptor trafficking, LEPROT. Overall, these data confirm the ability of FGF21 to reduce lipid accumulation in bovine liver and suggest the possibility that FGF21 does so by attenuating the hepatic influx of adipose tissue-derived fatty acids.
奶牛在泌乳早期通过从脂肪组织中大量且持续地动员脂肪酸来应对严重的能量不足。这种适应的一个不良副作用是肝脏中过多的脂质积累,这反过来又损害了肝脏功能。经历肝脂肪酸通量增加的小鼠通过新描述的激素成纤维细胞生长因子 21(FGF21)在肝脏和脂肪组织上的协调作用而免受这种情况的影响。FGF21 在血浆水平中的快速增加及其在泌乳早期的几个星期内持续升高表明它在奶牛中可能具有类似的作用。为了检验这一假设,在泌乳的 12.6 ± 2.2(±标准误差)天,奶牛被随机分配接受赋形剂(对照;n = 6)或重组人 FGF21(n = 7),首先是 3 毫克/公斤体重的 FGF21 推注,然后是 2 天后以 6.3 毫克/代谢体重/天的恒定静脉输注 FGF21,连续 9 天。推注后,人 FGF21 的半衰期为 194 分钟,其恒速输注使血浆总浓度增加 117 倍,超过了赋形剂输注奶牛的水平。FGF21 治疗对 9 天输注期间的自愿采食量、产奶量、奶能输出或净能平衡或最终体重均无影响。与对照组相比,在推注后 8 小时内,FGF21 组的循环血浆脂肪酸浓度较低,但在持续静脉输注期间,这种降低并不显著。在持续静脉输注结束时进行的肝活检中,FGF21 处理导致甘油三酯含量减少 50%,而不改变参与脂肪酸转运、酰基辅酶 A 激活或氧化的关键基因的 mRNA 丰度。相比之下,尽管生长激素有升高趋势,但 FGF21 治疗消除了对照组奶牛在 9 天静脉输注期间血浆胰岛素样生长因子 1 的恢复。这种作用与肝脏生长激素受体运输的细胞内抑制剂 LEPROT 的肝 mRNA 丰度增加有关。总的来说,这些数据证实了 FGF21 降低牛肝脏脂质积累的能力,并表明 FGF21 可能通过减弱脂肪组织衍生脂肪酸向肝脏的流入来实现这一作用。
