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在成年人中,以无酪氨酸、高苯丙氨酸摄入量进行的L-[1-¹³C]苯丙氨酸和L-[3,3-²H₂]酪氨酸的24小时静脉和口服示踪剂研究。

Twenty-four-hour intravenous and oral tracer studies with L-[1-13C]phenylalanine and L-[3,3-2H2]tyrosine at a tyrosine-free, generous phenylalanine intake in adults.

作者信息

Sanchez M, El-Khoury A E, Castillo L, Chapman T E, Basile Filho A, Beaumier L, Young V R

机构信息

Laboratory of Human Nutrition, Massachusetts Institute of Technology, Cambridge, 02142, USA.

出版信息

Am J Clin Nutr. 1996 Apr;63(4):532-45. doi: 10.1093/ajcn/63.4.532.

Abstract

The daily rates of whole-body phenylalanine oxidation and hydroxylation were determined in young men receiving [1-13C]phenylalanine and [2H2]tyrosine via primed, constant intravenous (n=3) or oral (n=5) infusion for 24 consecutive hours (12-h fast followed by 12-h fed period), and given a generous phenylalanine (100 mg.kg-1.d-1), tyrosine-free, but otherwise adequate L-amino acid-based diet for 6 d before the tracer study. Our hypothesis was that subjects would be in whole-body phenylalanine equilibrium. Estimates of the daily rates of phenylalanine oxidation (phe-ox) and hydroxylation (phe-OH) were significantly higher for the subjects receiving the oral compared with intravenous tracer (P<0.01 for both comparisons), with the estimates of phe-ox obtained with oral tracer during the 12-h fast period being close to those predicted from similar 24-h leucine kinetic studies. The precision of the agreement between the measured 24-h rates of phe-ox and phe-OH compared with the predicted daily rates by extrapolation from the last hour of the 12-h fast and fifth hour of the fed period was poor. From the 24-h data, daily phenylalanine balances were estimated to be positive for both the intravenous and oral tracer protocols, although it was less positive for the oral tracer group. These results imply that the [13C]phenylalanine probe underestimated whole-body irreversible loss of phenylalanine, and suggest that daily phenylalanine balance in earlier 24-h phenylalanine-tyrosine tracer studies at low phenylalanine intakes may have been overestimated. Studies involving [13C]tyrosine as tracer will be required to further assess whole-body aromatic amino acid balance.

摘要

在连续24小时(12小时禁食后接12小时进食期)接受[1-¹³C]苯丙氨酸和[²H₂]酪氨酸经初始负荷、持续静脉输注(n = 3)或口服输注(n = 5)的年轻男性中,测定全身苯丙氨酸氧化和羟化的每日速率。在示踪剂研究前6天,给予他们富含苯丙氨酸(100 mg·kg⁻¹·d⁻¹)、无酪氨酸但其他方面充足的基于L-氨基酸的饮食。我们的假设是受试者处于全身苯丙氨酸平衡状态。与静脉输注示踪剂的受试者相比,接受口服示踪剂的受试者苯丙氨酸氧化(phe-ox)和羟化(phe-OH)的每日速率估计值显著更高(两种比较均P<0.01),口服示踪剂在12小时禁食期获得的phe-ox估计值接近从类似的24小时亮氨酸动力学研究预测的值。与通过12小时禁食期最后一小时和进食期第五小时外推预测的每日速率相比,测量的24小时phe-ox和phe-OH速率之间的一致性精度较差。根据24小时数据,静脉输注和口服示踪剂方案的每日苯丙氨酸平衡估计均为正值,但口服示踪剂组的正值较小。这些结果表明,[¹³C]苯丙氨酸探针低估了苯丙氨酸的全身不可逆损失,并表明在早期低苯丙氨酸摄入量的24小时苯丙氨酸-酪氨酸示踪剂研究中,每日苯丙氨酸平衡可能被高估了。需要进行涉及[¹³C]酪氨酸作为示踪剂的研究,以进一步评估全身芳香族氨基酸平衡。

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