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β-羟基-β-甲基丁酸(HMB)改善杜氏肌营养不良犬的日常活动和全身蛋白质代谢:一项初步研究。

Beta-hydroxy-beta-methylbutyrate (HMB) improves daily activity and whole-body protein metabolism in Duchenne muscular dystrophy dogs: a pilot study.

作者信息

Nghiem Peter P, Rutledge Alexis M, Tehas Kyle, Kaderli Corine, Poling Meredith, Arnim Sidney, Dernov Vitaliy, van Sas Celine, Mackey Macie L, Have Gabriella A M Ten, Engelen Mariëlle P K J, Deutz Nicolaas E P

机构信息

Department of Veterinary Integrative Biosciences, Texas A&M University, College Station, TX, 77843-4458, USA.

Center for Translational Research in Aging and Longevity, Texas A&M University, College Station, TX, 77843, USA.

出版信息

Sci Rep. 2025 Feb 2;15(1):4026. doi: 10.1038/s41598-025-88651-8.

Abstract

Duchenne muscular dystrophy (DMD) is a severe neuromuscular disease due to loss of dystrophin, leading to progressive muscle wasting and physical inactivity. In this pilot study, we studied the effect of daily supplementation of the anabolic substrate beta-hydroxy-beta-methylbutyrate (HMB) on whole body protein and amino acid kinetics using novel isotope methods and daily activity in a canine model of DMD. Six DMD dogs were administered 3 g daily of HMB or placebo for 28 days according to a randomized, placebo-controlled, double-blinded crossover design. We measured pre- and post-intervention daily activity, biochemistry markers, and whole-body amino acid kinetics. We tracked daily activity with an activity monitoring device and measured plasma creatine kinase and standard clinical biochemistry panels to monitor muscle and organ function. To calculate whole body and intracellular amino acid production, we administered in the postabsorptive state an IV stable isotope solution containing 20 amino acid tracers. We collected blood before and six times after until two hours post tracer pulse administration and measured amino acid enrichments and concentrations by LC-MS/MS, subsequently followed by (non) compartmental modeling of the decay enrichment curves. Results were expressed as mean with 95% CI. Whole body production, plasma concentrations, and intra-/extracellular compartmental analyses of various amino acids were attenuated in HMB-dosed DMD dogs. Specifically, the plasma concentration of hydroxyproline (marker of collagen breakdown) was significantly higher in the placebo group compared to the HMB group. The intra- and extracellular pool sizes and flux between the two compartments of hydroxyproline was reduced in HMB treated dogs. DMD dogs treated with HMB as compared to placebo had a respective 40% increase in exertional (play) (951 [827, 1075] versus 569 [491, 647]; p < 0.0001) and 10.5% increase in non-exertional (active) activity (15,366 [14742, 15990] versus 13,806 [13148,14466]; p = 0.0016). In addition, a 6% reduction was found in rest time after HMB supplementation compared to placebo (23,857 [23,130, 24,584], versus 25,363 [24500, 26225]; p = 0.0122). Creatine kinase was not statistically different between groups. We did not observe any adverse clinical or biochemical-related effects of HMB dosing. Daily HMB supplementation in DMD dogs can safely and positively influence protein and amino acid metabolism and improve overall daily activity.

摘要

杜兴氏肌肉营养不良症(DMD)是一种严重的神经肌肉疾病,由于肌营养不良蛋白缺失,导致进行性肌肉萎缩和身体活动减少。在这项初步研究中,我们使用新型同位素方法研究了每日补充合成代谢底物β-羟基-β-甲基丁酸酯(HMB)对DMD犬模型全身蛋白质和氨基酸动力学以及日常活动的影响。根据随机、安慰剂对照、双盲交叉设计,给6只DMD犬每日服用3克HMB或安慰剂,持续28天。我们测量了干预前后的日常活动、生化指标和全身氨基酸动力学。我们使用活动监测设备跟踪日常活动,并测量血浆肌酸激酶和标准临床生化指标以监测肌肉和器官功能。为了计算全身和细胞内氨基酸的产生,我们在吸收后状态静脉注射含有20种氨基酸示踪剂的稳定同位素溶液。在注射示踪剂脉冲前和之后6次,直到注射后两小时采集血液,通过液相色谱-串联质谱法测量氨基酸富集度和浓度,随后对衰减富集曲线进行(非)房室建模。结果以均值和95%置信区间表示。在服用HMB的DMD犬中,各种氨基酸的全身产生、血浆浓度以及细胞内/外房室分析均减弱。具体而言,与HMB组相比,安慰剂组中羟脯氨酸(胶原蛋白分解的标志物)的血浆浓度显著更高。在接受HMB治疗的犬中,羟脯氨酸的细胞内和细胞外池大小以及两个房室之间的通量均降低。与安慰剂相比,接受HMB治疗的DMD犬的运动(玩耍)活动分别增加了40%(951 [827, 1075] 对569 [491, 647];p < 0.0001),非运动(主动)活动增加了10.5%(15,366 [14742, 15990] 对13,806 [13148,14466];p = 0.0016)。此外,与安慰剂相比,补充HMB后休息时间减少了6%(23,857 [23,130, 24,584] 对25,363 [24500, 26225];p = 0.0122)。两组之间肌酸激酶无统计学差异。我们未观察到服用HMB有任何不良临床或生化相关影响。在DMD犬中每日补充HMB可安全且积极地影响蛋白质和氨基酸代谢,并改善整体日常活动。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c538/11788438/65e125e82af2/41598_2025_88651_Fig1_HTML.jpg

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