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正常男性在6.0毫摩尔/升高血糖水平持续53小时后未出现糖毒性。

No glucotoxicity after 53 hours of 6.0 mmol/l hyperglycaemia in normal man.

作者信息

Flax H, Matthews D R, Levy J C, Coppack S W, Turner R C

机构信息

Diabetes Research Laboratories, Radcliffe Infirmary, Oxford, UK.

出版信息

Diabetologia. 1991 Aug;34(8):570-5. doi: 10.1007/BF00400275.

Abstract

In vitro and in vivo studies have suggested that metabolic deterioration can be induced by hyperglycaemia per se. The effect of 53 h of 2.2 mg glucose.kg ideal body weight-1.min-1 was examined in four normal male subjects. This produced overnight hyperglycaemia of 6.0 mmol/l on the two nights of the study compared with 4.7 mmol/l on the control night (p less than 0.05). In response there was a sustained, two-fold increase in basal plasma insulin (p less than 0.005) and C-peptide (p less than 0.05) levels. After two days of hyperglycaemia an increased Beta-cell response was demonstrated in response to an additional glucose infusion stimulus (estimated Beta-cell function median of 84% on the control day to 100% after two days glucose infusion). Plasma insulin and C-peptide responses to a 10.0 mmol/l hyperglycaemic clamp increased over the two days of the study (insulin from median 48 mU/l to 73 mU/l and C-peptide from median 2.0 pmol/ml to 2.6 pmol/l). Glucose tolerance to the additional glucose infusion stimulus improved, suggesting that the increased insulin response during hyperglycaemia was enhancing peripheral glucose uptake. The calculated peripheral insulin sensitivity was unchanged during the hyperglycaemic clamp. Thus, in response to the two days of basal hyperglycaemia, both the basal and stimulated Beta-cell responses were enhanced and there was no evidence for 'glucose toxicity' to the Beta-cells.

摘要

体外和体内研究表明,高血糖本身可导致代谢恶化。在4名正常男性受试者中,检测了以2.2毫克葡萄糖·千克理想体重-1·分钟-1的剂量持续输注53小时的效果。在研究的两个晚上,这导致夜间高血糖达到6.0毫摩尔/升,而对照夜为4.7毫摩尔/升(p<0.05)。作为反应,基础血浆胰岛素(p<0.005)和C肽(p<0.05)水平持续增加两倍。高血糖两天后,对额外葡萄糖输注刺激的β细胞反应增强(估计β细胞功能中位数从对照日的84%增加到葡萄糖输注两天后的100%)。在研究的两天中,血浆胰岛素和C肽对10.0毫摩尔/升高血糖钳夹的反应增加(胰岛素从中位数48毫单位/升增加到73毫单位/升,C肽从中位数2.0皮摩尔/毫升增加到2.6皮摩尔/升)。对额外葡萄糖输注刺激的葡萄糖耐量得到改善,表明高血糖期间胰岛素反应增加增强了外周葡萄糖摄取。在高血糖钳夹期间,计算得出的外周胰岛素敏感性没有变化。因此,在基础高血糖的两天期间,基础和刺激的β细胞反应均增强,没有证据表明β细胞存在“葡萄糖毒性”。

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