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正常大鼠和糖尿病大鼠胰岛组织中的葡萄糖和三磷酸腺苷水平。

Glucose and ATP levels in pancreatic islet tissue of normal and diabetic rats.

作者信息

Matschinsky F M, Pagliara A S, Stillings S N, Hover B A

出版信息

J Clin Invest. 1976 Nov;58(5):1193-200. doi: 10.1172/JCI108572.

Abstract

It has been suggested that the hyperglucagonemia observed in diabetic animals and man may be due to an impairment of glucose uptake and metabolism by the alpha-cells resulting in a decreased production of ATP. To test this hypothesis glucose, ATP, glucagon, and insulin were measured in pancreatic islets of normal and alloxan or streptozotocin diabetic rats. Two experimental approaches were used. In the first, the pancreas was perfused in vitro for assessing insulin and glucagon release due to 10 mM amino acids with and without 5 mM glucose. These perfusions were performed in the presence and absence of insulin. After perfusion, the pancreas was frozen and processed for analysis of islet glucose, ATP, insulin, and glucagon content. The second approach was to investigate the islet sucrose, urea, and glucose spaces together with ATP, insulin, and glucagon content in vivo in normal and in insulin-treated and untreated streptozotocin diabetic rats. Perfusion of the pancreas in vitro with 5 mM glucose resulted in higher glucose content of normal islets than in alloxan and streptozotocin diabetic islets. Similarly in the in vivo studies, the intracellular glucose space of the streptozotocin diabetic islets was 30% the value found in normals. In the in vivo experiments, despite the relatively small intracellular glucose space of alpha-cell islets, the ATP content of these islets was only 15-20% lower than the ATP content of normal islets. In the in vitro experiments, perfusion with glucose resulted in ATP contents of alpha-cell islets and of normal mixed alpha-beta-cell islets which were indistinguishable. However, the ATP content of alpha-cell islets was maintained for prolonged periods in the absence of glucose in contrast to mixed islets, composed primarily of beta-cells, in which the ATP level decreased by 45% when glucose-free medium was perfused for sustained periods. Finally, insulin infused in high concentrations or administered to the diabetic animal had no effect on the glucose spaces or the ATP contents of normal or alpha-cell islets. It can be calculated that in vivo the intracellular glucose level of islets from streptozotocin treated rats is approximately 15 mM. Since in normals an extracellular glucose concentration of this magnitude inhibits stimulated glucagon release completely, it would seem unlikely that a lack of intracellular glucose is the cause of the apparent glucose "blindness" of the alpha-cells in diabetes. In fact, in perfusion studies as little as 2.5 mM free intracellular glucose was sufficient to suppress glucagon secretion from diabetic alpha-cells. The results of the ATP measurements clearly eliminate a possible energy deficit of diabetic alpha-cells as cause of the apparent glucose resistance of alpha-cells.

摘要

有人提出,在糖尿病动物和人类中观察到的高胰高血糖素血症可能是由于α细胞对葡萄糖的摄取和代谢受损,导致ATP生成减少。为了验证这一假设,对正常大鼠以及用四氧嘧啶或链脲佐菌素诱导糖尿病的大鼠的胰岛中的葡萄糖、ATP、胰高血糖素和胰岛素进行了测量。采用了两种实验方法。第一种方法是在体外灌注胰腺,以评估在有和没有5 mM葡萄糖存在的情况下,10 mM氨基酸引起的胰岛素和胰高血糖素释放。这些灌注在有和没有胰岛素的情况下进行。灌注后,将胰腺冷冻并进行处理,以分析胰岛中的葡萄糖、ATP、胰岛素和胰高血糖素含量。第二种方法是在正常大鼠、胰岛素治疗和未治疗的链脲佐菌素糖尿病大鼠体内研究胰岛蔗糖、尿素和葡萄糖空间以及ATP、胰岛素和胰高血糖素含量。在体外向胰腺灌注5 mM葡萄糖后,正常胰岛中的葡萄糖含量高于四氧嘧啶和链脲佐菌素糖尿病胰岛中的葡萄糖含量。同样,在体内研究中,链脲佐菌素糖尿病胰岛的细胞内葡萄糖空间是正常胰岛的30%。在体内实验中,尽管α细胞胰岛的细胞内葡萄糖空间相对较小,但这些胰岛的ATP含量仅比正常胰岛的ATP含量低15 - 20%。在体外实验中,用葡萄糖灌注导致α细胞胰岛和正常α-β混合细胞胰岛的ATP含量没有差异。然而,与主要由β细胞组成的混合胰岛不同,α细胞胰岛在无葡萄糖的情况下ATP含量能长时间维持,当用无葡萄糖培养基持续灌注时,混合胰岛的ATP水平会下降45%。最后,高浓度输注胰岛素或给糖尿病动物注射胰岛素对正常或α细胞胰岛的葡萄糖空间或ATP含量没有影响。可以计算出,在体内,链脲佐菌素处理大鼠的胰岛细胞内葡萄糖水平约为15 mM。由于在正常情况下,这种程度的细胞外葡萄糖浓度会完全抑制刺激后的胰高血糖素释放,因此糖尿病中α细胞明显的葡萄糖“盲目性”似乎不太可能是由于细胞内葡萄糖缺乏所致。事实上,在灌注研究中,低至2.5 mM的细胞内游离葡萄糖就足以抑制糖尿病α细胞分泌胰高血糖素。ATP测量结果清楚地排除了糖尿病α细胞可能存在的能量不足是α细胞明显葡萄糖抵抗的原因。

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