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胰高血糖素输注改变犬的循环代谢组和尿氨基酸排泄。

Glucagon infusion alters the circulating metabolome and urine amino acid excretion in dogs.

机构信息

Loftus Laboratory, Department of Clinical Sciences, Cornell University, College of Veterinary Medicine, Ithaca, New York, USA.

VCA Colonial Animal Hospital, Ithaca, New York, USA.

出版信息

J Endocrinol. 2024 Jun 27;262(2). doi: 10.1530/JOE-24-0051. Print 2024 Aug 1.

Abstract

Glucagon plays a central role in amino acid (AA) homeostasis. The dog is an established model of glucagon biology, and recently, metabolomic changes in people associated with glucagon infusions have been reported. Glucagon also has effects on the kidney; however, changes in urinary AA concentrations associated with glucagon remain under investigation. Therefore, we aimed to fill these gaps in the canine model by determining the effects of glucagon on the canine plasma metabolome and measuring urine AA concentrations. Employing two constant rate glucagon infusions (CRI) - low-dose (CRI-LO: 3 ng/kg/min) and high-dose (CRI-HI: 50 ng/kg/min) on five research beagles, we monitored interstitial glucose and conducted untargeted liquid chromatography-tandem mass spectrometry (LC-MS/MS) on plasma samples and urine AA concentrations collected pre- and post-infusion. The CRI-HI induced a transient glucose peak (90-120 min), returning near baseline by infusion end, while only the CRI-LO resulted in 372 significantly altered plasma metabolites, primarily reductions (333). Similarly, CRI-HI affected 414 metabolites, with 369 reductions, evidenced by distinct clustering post-infusion via data reduction (PCA and sPLS-DA). CRI-HI notably decreased circulating AA levels, impacting various AA-related and energy-generating metabolic pathways. Urine analysis revealed increased 3-methyl-l-histidine and glutamine, and decreased alanine concentrations post-infusion. These findings demonstrate glucagon's glucose-independent modulation of the canine plasma metabolome and highlight the dog's relevance as a translational model for glucagon biology. Understanding these effects contributes to managing dysregulated glucagon conditions and informs treatments impacting glucagon homeostasis.

摘要

胰高血糖素在氨基酸(AA)稳态中发挥核心作用。狗是胰高血糖素生物学的既定模型,最近,与胰高血糖素输注相关的人体内代谢组学变化已经报道。胰高血糖素对肾脏也有影响;然而,与胰高血糖素相关的尿液 AA 浓度变化仍在研究中。因此,我们旨在通过确定胰高血糖素对犬血浆代谢组的影响并测量尿液 AA 浓度来填补犬模型中的这些空白。在五只研究用比格犬上进行了两次恒速胰高血糖素输注(CRI)-低剂量(CRI-LO:3ng/kg/min)和高剂量(CRI-HI:50ng/kg/min),监测间质葡萄糖,并在输注前后采集血浆样本和尿液 AA 浓度进行非靶向液相色谱-串联质谱(LC-MS/MS)分析。CRI-HI 诱导短暂的葡萄糖峰值(90-120 分钟),输注结束时接近基线,而仅 CRI-LO 导致 372 种显著改变的血浆代谢物,主要是减少(333)。同样,CRI-HI 影响 414 种代谢物,其中 369 种减少,输注后通过数据减少(PCA 和 sPLS-DA)可明显看出聚类。CRI-HI 显著降低循环 AA 水平,影响各种 AA 相关和能量生成代谢途径。尿液分析显示输注后 3-甲基-L-组氨酸和谷氨酰胺增加,丙氨酸浓度降低。这些发现表明胰高血糖素对犬血浆代谢组的葡萄糖非依赖性调节,并强调了犬作为胰高血糖素生物学转化模型的相关性。了解这些影响有助于控制失调的胰高血糖素状况,并为影响胰高血糖素稳态的治疗提供信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/24c1/11301426/06450af81342/JOE-24-0051fig1.jpg

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