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在多次给予低剂量链脲佐菌素的小鼠中,胰岛质量和B细胞功能的重大损失先于高血糖出现。

A major loss in islet mass and B-cell function precedes hyperglycemia in mice given multiple low doses of streptozotocin.

作者信息

Bonnevie-Nielsen V, Steffes M W, Lernmark A

出版信息

Diabetes. 1981 May;30(5):424-9. doi: 10.2337/diab.30.5.424.

Abstract

Streptozotocin (SZ) given in five low doses causes diabetes and an associated lymphocytic infiltration of the pancreatic islets. Using C57BL/KsJ-mice, we demonstrate a reduction in islet number (--38%) and volume (--64%) within 1 day following the last injection of SZ. A substantial fall of insulin secretory capacity (--84%) in the in vitro perfused pancreas matches the reduction in islet cell volume. The parameters of decreased islet function seem to precede the peak of lymphocytic infiltration, occurring 3 days after the last dose of SZ. These functional changes are readily demonstrable before a rise in fasting blood glucose, but they seem to be reflected more readily by a rise in nonfasting blood glucose levels. With development of overt diabetes, as measured by elevated fasting and nonfasting glucose levels, the measures of islet volume and function are reduced to levels only 1--2% of those found in control mice. Taken together, these observations reflect a rapid, islet-toxic effect of SZ that substantially decreases insulin secretory capacity. When islet function falls more than 90%, blood glucose levels begin to reflect the pathophysiologic process. In many aspects, the low-dose SZ model of diabetes parallels the development of diabetes in man. If so, measures other than blood sugar must be developed to identify at an early stage processes reducing islet volume and function.

摘要

连续五次给予低剂量链脲佐菌素(SZ)可导致糖尿病以及胰岛的淋巴细胞浸润。利用C57BL/KsJ小鼠,我们发现在最后一次注射SZ后的1天内,胰岛数量减少了38%,体积减少了64%。体外灌注胰腺中胰岛素分泌能力大幅下降(84%),这与胰岛细胞体积的减少相匹配。胰岛功能下降的参数似乎在淋巴细胞浸润达到峰值之前出现,淋巴细胞浸润在最后一剂SZ注射后3天出现。这些功能变化在空腹血糖升高之前就很容易被检测到,但它们似乎更容易通过非空腹血糖水平的升高反映出来。随着明显糖尿病的发展,通过空腹和非空腹血糖水平升高来衡量,胰岛体积和功能的指标降低到仅为对照小鼠的1% - 2%。综上所述,这些观察结果反映了SZ对胰岛的快速毒性作用,该作用显著降低了胰岛素分泌能力。当胰岛功能下降超过90%时,血糖水平开始反映病理生理过程。在许多方面,低剂量SZ糖尿病模型与人类糖尿病的发展相似。如果是这样,必须开发除血糖之外的其他指标来早期识别导致胰岛体积和功能降低的过程。

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