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使用L-[1-14C]酪氨酸进行代谢研究,以探究一种用于通过正电子发射断层扫描(PET)测量蛋白质合成速率的动力学模型。

Metabolic studies with L-[1-14C]tyrosine for the investigation of a kinetic model to measure protein synthesis rates with PET.

作者信息

Ishiwata K, Vaalburg W, Elsinga P H, Paans A M, Woldring M G

机构信息

Department of Nuclear Medicine, University Hospital, Groningen, The Netherlands.

出版信息

J Nucl Med. 1988 Apr;29(4):524-9.

PMID:3258366
Abstract

To evaluate a kinetic model for measuring protein synthesis rates by positron emission tomography (PET) in neoplastic and normal tissue, metabolic studies with L-[1-14C]tyrosine were carried out. As an animal model, rats bearing Walker 256 carcinosarcoma were used. Within 60 min after injection, several metabolic parameters were measured. The highest radioactivity uptake, expressed as the differential absorption ratio, was found in pancreas, followed by liver, tumor, and brain. A rapid decarboxylation was observed during the first 15 min. After 60 min, 7.4% of the total injected 14C was expired as 14CO2. In plasma a significant amount of [14C]bicarbonate was detected, but in tissue the amount was negligible. Protein incorporation increased with time. The incorporation rate was the highest in the liver followed by pancreas, tumor, and brain tissues. At 60 min after injection, more than approximately 80% of the 14C in tissue was protein bound. In plasma after a rapid clearance during the first 15 min, the total 14C level increased rapidly and paralleled the increase of protein-bound 14C. As nonprotein [14C]metabolites, in plasma, tumor and brain tissues, p-hydroxyphenylpyruvic acid, p-hydroxyphenyllactic acid, and unidentified metabolites were observed by high performance liquid chromatography. The formation of 14C-labeled 3,4-dihydroxyphenylalanine was found to be negligible. The total amount of these nonprotein metabolites increased with time. At 60 min after injection the percentages of the total nonprotein metabolites and [14C]bicarbonate were only 5.0%, 1.9%, and 3.7% in plasma, tumor and brain tissue, respectively. From our data it is concluded that [11C]carboxylic-labeled tyrosine would be a suitable radiopharmaceutical for measuring protein synthesis rates in neoplastic and normal tissue by PET.

摘要

为了评估通过正电子发射断层扫描(PET)测量肿瘤组织和正常组织中蛋白质合成速率的动力学模型,进行了L-[1-14C]酪氨酸的代谢研究。以携带Walker 256癌肉瘤的大鼠作为动物模型。注射后60分钟内,测量了几个代谢参数。以微分吸收比表示的最高放射性摄取出现在胰腺,其次是肝脏、肿瘤和大脑。在最初的15分钟内观察到快速脱羧。60分钟后,注入的总14C中有7.4%以14CO2形式呼出。在血浆中检测到大量的[14C]碳酸氢盐,但在组织中该量可忽略不计。蛋白质掺入随时间增加。掺入率在肝脏中最高,其次是胰腺、肿瘤和脑组织。注射后60分钟,组织中超过约80%的14C与蛋白质结合。在血浆中,最初15分钟快速清除后,总14C水平迅速升高,并与蛋白质结合的14C的增加平行。作为非蛋白质[14C]代谢物,通过高效液相色谱法在血浆、肿瘤和脑组织中观察到对羟基苯丙酮酸、对羟基苯乳酸和未鉴定的代谢物。发现14C标记的3,4-二羟基苯丙氨酸的形成可忽略不计。这些非蛋白质代谢物的总量随时间增加。注射后60分钟,血浆、肿瘤和脑组织中总非蛋白质代谢物和[14C]碳酸氢盐的百分比分别仅为5.0%、1.9%和3.7%。根据我们的数据得出结论,[11C]羧基标记的酪氨酸将是一种适合通过PET测量肿瘤组织和正常组织中蛋白质合成速率的放射性药物。

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