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通过[15N]精氨酸到[15N]瓜氨酸的标记来测定健康男性的全身一氧化氮合成。

Whole body nitric oxide synthesis in healthy men determined from [15N] arginine-to-[15N]citrulline labeling.

作者信息

Castillo L, Beaumier L, Ajami A M, Young V R

机构信息

Laboratory of Human Nutrition, Massachusetts Institute of Technology, Cambridge 02139, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Oct 15;93(21):11460-5. doi: 10.1073/pnas.93.21.11460.

Abstract

The rates of whole body nitric oxide (NO) synthesis, plasma arginine flux, and de novo arginine synthesis and their relationships to urea production, were examined in a total of seven healthy adults receiving an L-amino acid diet for 6 days. NO synthesis was estimated by the rate of conversion of the [15N] guanidino nitrogen of arginine to plasma [15N] ureido citrulline and compared with that based on urinary nitrite (NO2-)/nitrate (NO3-) excretion. Six subjects received on dietary day 7, a 24-hr (12-hr fed/12-hr fasted) primed, constant, intravenous infusion of L-[guanidino-15N2]arginine and [13C]urea. A similar investigation was repeated with three of these subjects, plus an additional subject, in which they received L-[ureido-13C]citrulline, to determine plasma citrulline fluxes. The estimated rates (mean +/- SD) of NO synthesis over a period of 24 hr averaged 0.96 +/- 0.1 mumol .kg-1.hr-1 and 0.95 +/- 0.1 mumol.kg-1.hr-1, for the [15N]citrulline and the nitrite/nitrate methods, respectively. About 15% of the plasma arginine turnover was associated with urea formation and 1.2% with NO formation. De novo arginine synthesis averaged 9.2 +/- 1.4 mumol. kg-1.hr-1, indicating that approximately 11% of the plasma arginine flux originates via conversion of plasma citrulline to arginine. Thus, the fraction of the plasma arginine flux associated with NO and also urea synthesis in healthy humans is small, although the plasma arginine compartment serves as a significant precursor pool (54%) for whole body NO formation. This tracer model should be useful for exploring these metabolic relationships in vivo, under specific pathophysiologic states where the L-arginine-NO pathway might be altered.

摘要

对总共7名接受L-氨基酸饮食6天的健康成年人,检测了全身一氧化氮(NO)合成率、血浆精氨酸通量、从头合成精氨酸及其与尿素生成的关系。通过精氨酸的[15N]胍基氮向血浆[15N]脲基瓜氨酸的转化速率估算NO合成,并与基于尿中亚硝酸盐(NO2-)/硝酸盐(NO3-)排泄的估算值进行比较。6名受试者在饮食第7天接受24小时(12小时进食/12小时禁食)的L-[胍基-15N2]精氨酸和[13C]尿素的首剂量、持续静脉输注。对其中3名受试者及另一名受试者重复进行了类似研究,他们接受L-[脲基-13C]瓜氨酸,以测定血浆瓜氨酸通量。[15N]瓜氨酸法和亚硝酸盐/硝酸盐法在24小时内的NO合成估算率(均值±标准差)分别平均为0.96±0.1μmol·kg-1·hr-1和0.95±0.1μmol·kg-1·hr-1。约15%的血浆精氨酸周转与尿素生成有关,1.2%与NO生成有关。从头合成精氨酸平均为9.2±1.4μmol·kg-1·hr-1,表明约11%的血浆精氨酸通量源自血浆瓜氨酸向精氨酸的转化。因此,在健康人体内,与NO和尿素合成相关的血浆精氨酸通量比例较小,尽管血浆精氨酸池是全身NO形成的重要前体池(54%)。该示踪模型对于在体内探索特定病理生理状态下L-精氨酸-NO途径可能改变时的这些代谢关系应是有用的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1372/38079/ad506113c1e4/pnas01525-0188-a.jpg

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