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体内人体叶酸代谢的定量分析。

Quantitation of in vivo human folate metabolism.

作者信息

Lin Yumei, Dueker Stephen R, Follett Jennifer R, Fadel James G, Arjomand Ali, Schneider Philip D, Miller Joshua W, Green Ralph, Buchholz Bruce A, Vogel John S, Phair Robert D, Clifford Andrew J

机构信息

Departments of Nutrition and Pathology Department, University of California-Davis, One Shields Avenue,. Davis. CA 95616-8669, USA.

出版信息

Am J Clin Nutr. 2004 Sep;80(3):680-91. doi: 10.1093/ajcn/80.3.680.

Abstract

BACKGROUND

A quantitative understanding of human folate metabolism is needed.

OBJECTIVE

The objective was to quantify and interpret human folate metabolism as it might occur in vivo.

DESIGN

Adults (n = 13) received 0.5 nmol [(14)C]pteroylmonoglutamate (100 nCi radioactivity) plus 79.5 nmol pteroylmonoglutamate in water orally. (14)C was measured in plasma, erythrocytes, urine, and feces for >/=40 d. Kinetic modeling was used to analyze and interpret the data.

RESULTS

According to the data, the population was healthy and had a mean dietary folate intake of 1046 nmol/d, and the apparent dose absorption of (14)C was 79%. The model predictions showed that only 0.25% of plasma folate was destined for marrow, mean bile folate flux was 5351 nmol/d, and the digestibility of the mix (1046 + 5351 nmol/d) was 92%. About 33% of visceral pteroylmonoglutamate was converted to the polyglutamate form, most of the body folate was visceral (>99%), most of the visceral folate was pteroylpolyglutamate (>98%), total body folate was 225 micromol, and pteroylpolyglutamate synthesis, recycling, and catabolism were 1985, 1429, and 556 nmol/d, respectively. Mean residence times were 0.525 d as visceral pteroylmonoglutamate, 119 d as visceral pteroylpolyglutamate, 0.0086 d as plasma folate, and 0.1 d as gastrointestinal folate.

CONCLUSIONS

Across subjects, folate absorption, bile folate flux, and body folate stores were larger than prior estimates. Marrow folate uptake and pteroylpolyglutamate synthesis, recycling, and catabolism are saturable processes. Visceral pteroylpolyglutamate was an immediate precursor of plasma p-aminobenzoylglutamate. The model is a working hypothesis with derived features that are explicitly model-dependent. It successfully quantitated folate metabolism, encouraging further rigorous testing.

摘要

背景

需要对人体叶酸代谢进行定量了解。

目的

目的是对人体叶酸代谢在体内可能的发生情况进行定量和解释。

设计

13名成年人经口摄入0.5纳摩尔[¹⁴C]蝶酰单谷氨酸(放射性为100纳居里)加79.5纳摩尔蝶酰单谷氨酸的水溶液。在40多天内对血浆、红细胞、尿液和粪便中的¹⁴C进行测量。采用动力学模型分析和解释数据。

结果

根据数据,该人群健康,膳食叶酸平均摄入量为1046纳摩尔/天,¹⁴C的表观剂量吸收率为79%。模型预测显示,只有0.25%的血浆叶酸进入骨髓,胆汁叶酸平均通量为5351纳摩尔/天,混合物(1046 + 5351纳摩尔/天)的消化率为92%。约33%的内脏蝶酰单谷氨酸转化为多谷氨酸形式,体内大部分叶酸存在于内脏(>99%),大部分内脏叶酸为蝶酰多谷氨酸(>98%),全身叶酸总量为225微摩尔,蝶酰多谷氨酸的合成、再循环和分解代谢分别为1985、1429和556纳摩尔/天。内脏蝶酰单谷氨酸的平均停留时间为0.525天,内脏蝶酰多谷氨酸为119天,血浆叶酸为0.0086天,胃肠道叶酸为0.1天。

结论

在不同个体中,叶酸吸收、胆汁叶酸通量和体内叶酸储备均高于先前估计。骨髓叶酸摄取以及蝶酰多谷氨酸的合成、再循环和分解代谢是可饱和过程。内脏蝶酰多谷氨酸是血浆对氨基苯甲酰谷氨酸的直接前体。该模型是一个具有明确依赖模型特征的工作假设。它成功地对叶酸代谢进行了定量,有助于进一步进行严格测试。

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