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肿瘤进行性生长大鼠氨基酸动力学的改变

Altered amino acid kinetics in rats with progressive tumor growth.

作者信息

Kawamura I, Moldawer L L, Keenan R A, Batist G, Bothe A, Bistrian B R, Blackburn G L

出版信息

Cancer Res. 1982 Mar;42(3):824-9.

PMID:7059980
Abstract

The present study was designed to determine whether alterations in host metabolism associated with progressive tumor growth were a result of the anorexia frequently observed with cancer or could be attributed to other direct tumor effects. Rates of tyrosine flux, oxidation, and incorporation into protein, as well as fractional protein-synthetic rates in nonsecretory liver, muscle, and tumor, were determined in overnight-fasted rats, 5 to 6 (Stage I), 10 to 11 (Stage II), and 15 to 16 (Stage III) days following s.c. implantation of RNC-254 fibrosarcoma. Tumor-bearing rats were allowed to consume a purified diet containing 20% protein ad libitum, and results were compared to non-tumor-bearing rats pair fed quantities of food equivalent to tumor-bearing animals or allowed to consume the diet ad libitum. Results demonstrate that during later stages of tumor growth (Stage III) calorie intake and nontumor body weight gain were reduced in tumor-bearing rats (p less than 0.05). Fifteen and 16 days following implantation, there were significant changes in amino acid kinetics that were not observed after earlier periods of tumor growth and that could not be explained by any reduction in dietary intake. Rates of tyrosine appearance in the plasma and subsequent incorporation into whole-body protein were increased 33 and 34%, respectively (p less than 0.05), when compared to non-tumor-bearing rats fed equivalent quantities of food. Whole-body tyrosine oxidation rates were unchanged. Skeletal protein synthesis, as reflected by gastrocnemius or rectus abdominus muscle, was reduced from 10.5 and 10.1%/day to 7.4 and 6.0%/day, respectively (p less than 0.05), in tumor-bearing compared to pair-fed animals. The findings suggest that significant alterations in protein metabolism occur in advanced stages of experimental neoplastic disease which cannot be explained by reductions in dietary intake and are aimed at providing adequate quantities of endogenous amino acids for net tumor growth.

摘要

本研究旨在确定与肿瘤进行性生长相关的宿主代谢改变是癌症常见的厌食症所致,还是可归因于肿瘤的其他直接作用。在禁食过夜的大鼠中,于皮下植入RNC - 254纤维肉瘤后的5至6天(I期)、10至11天(II期)和15至16天(III期),测定了酪氨酸通量、氧化以及掺入蛋白质的速率,以及非分泌性肝脏、肌肉和肿瘤中的蛋白质合成分数速率。让荷瘤大鼠随意食用含20%蛋白质的纯化饮食,并将结果与成对喂食等量食物的非荷瘤大鼠或随意食用该饮食的非荷瘤大鼠进行比较。结果表明,在肿瘤生长的后期阶段(III期),荷瘤大鼠的卡路里摄入量和非肿瘤体重增加减少(p<0.05)。植入后15天和16天,氨基酸动力学发生了显著变化,这在肿瘤生长早期未观察到,且无法用饮食摄入量的任何减少来解释。与喂食等量食物的非荷瘤大鼠相比,血浆中酪氨酸的出现速率和随后掺入全身蛋白质的速率分别增加了33%和34%(p<0.05)。全身酪氨酸氧化速率未改变。与成对喂食的动物相比,荷瘤大鼠腓肠肌或腹直肌所反映的骨骼肌蛋白质合成分别从每天10.5%和10.1%降至7.4%和6.0%(p<0.05)。这些发现表明,在实验性肿瘤疾病的晚期阶段,蛋白质代谢发生了显著改变,这无法用饮食摄入量的减少来解释,其目的是为肿瘤净生长提供足够数量的内源性氨基酸。

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