与年轻人相比，中年人的亮氨酸转氨作用较低。

Department of Medicine, Division of Metabolic Diseases, University of Padova, Padova, Italy

J Nutr. 2017 Nov;147(11):2025-2030. doi: 10.3945/jn.117.250852. Epub 2017 Sep 20.

Insulin and age affect leucine (and protein) kinetics in vivo. However, to our knowledge, leucine transamination and the effects of insulin have not been studied in participants of different ages. The aims of the study were to measure whole-body leucine deamination to α-ketoisocaproate (KIC) and KIC reamination to leucine in middle-aged and younger healthy adults, both in the postabsorptive state and after hyperinsulinemia. Younger (mean ± SE age: 26 ± 2 y) and middle-aged (54 ± 3 y) healthy men and women were enrolled. Isotope dilution methods with 2 independent leucine and KIC tracers, a dual isotope model and the euglycemic, hyperinsulinemic clamp technique, were used. Leucine deamination [expressed as μmol/(kg × min)] was consistently greater than KIC reamination. In middle-aged adults, postabsorptive leucine deamination (0.77 ± 0.05), reamination (0.49 ± 0.04), and net deamination (0.28 ± 0.04) were ∼30% lower than in the younger group (deamination: 1.12 ± 0.07; reamination: 0.70 ± 0.09; net deamination: 0.42 ± 0.04) ( < 0.002, < 0.05, and < 0.015, respectively). After the hyperinsulinemic clamp, plasma leucine and KIC concentrations were reduced by ∼50% in both groups. Deamination and reamination also were suppressed by ∼40-50% in both groups ( < 0.001); however, they remained lower [-35% ( = 0.02) and -25% ( = 0.036), respectively] in the middle-aged than in the younger participants. The leucine rate of appearance and its suppression by insulin were similar in the middle-aged and in the younger subjects. By using both the basal and the clamp data, deamination was directly correlated with the plasma leucine concentration ( = 0.61, < 0.0025) and reamination to that of plasma KIC ( = 0.79, < 0.00002). Expressing the data relative to lean body mass did not substantially alter the results. Leucine deamination and reamination are lower in middle-aged than in younger adults, both in the postabsorptive and in the insulin-stimulated state. In middle age, a decreased net leucine transamination may represent a mechanism to spare this essential amino acid.

胰岛素和年龄会影响体内亮氨酸（及蛋白质）的动力学。然而，据我们所知，不同年龄参与者的亮氨酸转氨作用及胰岛素的影响尚未得到研究。本研究的目的是测量中年和青年健康成年人在空腹状态及高胰岛素血症后，全身亮氨酸向α-酮异己酸（KIC）的脱氨作用以及KIC向亮氨酸的再氨化作用。招募了青年（平均±标准误年龄：26±2岁）和中年（54±3岁）的健康男性和女性。使用了带有两种独立亮氨酸和KIC示踪剂的同位素稀释法、双同位素模型以及正常血糖、高胰岛素钳夹技术。亮氨酸脱氨作用[以μmol/(kg×min)表示]始终大于KIC再氨化作用。在中年成年人中，空腹状态下的亮氨酸脱氨作用（0.77±0.05）、再氨化作用（0.49±0.04）和净脱氨作用（0.28±0.04）比青年组低约30%（脱氨作用：1.12±0.07；再氨化作用：0.70±0.09；净脱氨作用：0.42±0.04）（分别为<0.002、<0.05和<0.015）。高胰岛素钳夹后，两组血浆亮氨酸和KIC浓度均降低了约50%。两组的脱氨作用和再氨化作用也均被抑制了约40% - 50%（<0.001）；然而，中年参与者的脱氨作用和再氨化作用仍低于青年参与者[分别低-35%（P = 0.02）和-25%（P = 0.036）]。中年和青年受试者的亮氨酸出现率及其受胰岛素的抑制情况相似。综合基础数据和钳夹数据来看，脱氨作用与血浆亮氨酸浓度直接相关（r = 0.61，P < 0.0025），再氨化作用与血浆KIC浓度直接相关（r = 0.79，P < 0.00002）。以瘦体重为参照来表示数据，结果并未有实质性改变。在空腹状态和胰岛素刺激状态下，中年人的亮氨酸脱氨作用和再氨化作用均低于青年人。在中年时期，亮氨酸净转氨作用降低可能是一种节约这种必需氨基酸的机制。