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营养物质摄入的速率和途径对蛋白质代谢的影响。

The effects of rate and route of nutrient intake on protein metabolism.

作者信息

Enrione E B, Gelfand M J, Morgan D, Sperling M, Wagner S C, Popp M B

出版信息

J Surg Res. 1986 Apr;40(4):320-5. doi: 10.1016/0022-4804(86)90194-0.

Abstract

Isotopic measurements of protein kinetics are useful for the investigation of metabolic protein disorders during surgical illness. The effects of rate and route (oral vs parenteral) of nutritional substrate intake have not been well defined. Fischer 344 rats were infused with a total parenteral nutrition (TPN) solution at either 25, 100, or 175% of their normal substrate intake or were fed an oral diet ad libitum. After 4 days, [15N]glycine was infused at 0.138 mg 15N/hr for 24 hr. Whole-body protein turnover (WPT), synthesis, and catabolism were determined by 15N urea enrichment. Fractional synthesis rates (FSR) of liver and muscle protein were calculated by analyzing 15N tissue enrichment. WPT (r = 0.93, P less than 0.001) and liver FSR (r = 0.57, P less than 0.01) increased linearly with TPN infusion rates. All rats had protein synthesis rates greater than catabolism rates except for the rats infused with 25% TPN. Although caloric intake was the same in rats fed orally and those infused with 100% TPN, the orally fed rats had faster WPT (P less than 0.001), synthesis (P less than 0.05), catabolism (P less than 0.001), and liver FSR (P less than 0.05) than the TPN rats. Muscle FSR was not significantly affected by either the route of feeding or the TPN infusion rate. In this study, rate and route of substrate intake affected protein kinetics in the whole animal and liver, but not in muscle. Rate and route of nutrient intake need to be carefully specified and controlled during isotopic studies of protein kinetics.

摘要

蛋白质动力学的同位素测量对于研究外科疾病期间的代谢性蛋白质紊乱很有用。营养底物摄入的速率和途径(口服与胃肠外)的影响尚未明确界定。给Fischer 344大鼠输注全胃肠外营养(TPN)溶液,输注量分别为其正常底物摄入量的25%、100%或175%,或者随意给予口服饮食。4天后,以0.138 mg 15N/小时的速率输注[15N]甘氨酸24小时。通过15N尿素富集测定全身蛋白质周转率(WPT)、合成和分解代谢。通过分析15N组织富集计算肝脏和肌肉蛋白质的分数合成率(FSR)。WPT(r = 0.93,P < 0.001)和肝脏FSR(r = 0.57,P < 0.01)随TPN输注速率呈线性增加。除了输注25% TPN的大鼠外,所有大鼠的蛋白质合成率均大于分解代谢率。尽管口服喂养的大鼠和输注100% TPN的大鼠热量摄入相同,但口服喂养的大鼠比TPN喂养的大鼠具有更快的WPT(P < 0.001)、合成(P < 0.05)、分解代谢(P < 0.001)和肝脏FSR(P < 0.05)。肌肉FSR不受喂养途径或TPN输注速率的显著影响。在本研究中,底物摄入的速率和途径影响整个动物和肝脏的蛋白质动力学,但不影响肌肉。在蛋白质动力学的同位素研究期间,营养摄入的速率和途径需要仔细确定和控制。

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