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单核细胞对胰岛素的降解作用。

Insulin degradation by mononuclear cells.

作者信息

Powers A C, Solomon S S, Duckworth W C

出版信息

Diabetes. 1980 Jan;29(1):27-32. doi: 10.2337/diab.29.1.27.

Abstract

Mononuclear cells from peripheral blood possess insulin receptors that are altered in number or binding affinity in certain metabolic diseases as obesity. The monocyte, and not the lymphocyte, is the cell with the capacity to specifically bind insulin. Furthermore, this binding appears to mirror the receptor status on such insulin target tissues as liver, muscle, and fat. Since liver, muscle, and fat also degrade insulin, mononuclear cells from the blood of normal volunteers were examined for insulin-degrading activity. Intact cells were incubated with 125I-insulin and the amount of degraded insulin was measured by the trichloroacetic acid-precipitation technique. Insulin-degrading activity increased when the number of cells and the time of incubation were increased. Total insulin binding behaved in a similar fashion. Very little degradation was seen at 4 degrees or 15 degrees. The Km for insulin-degrading activity was 7.03 X 10(-8) M. Homogenized mononuclear cells degraded two to five times more insulin than did intact cells and also demonstrated cell concentration, time, and temperature dependence for degradation. The Km of degradation for homogenized mononuclear cells was 2.2 X 10(-8) M. Subcellular fractionation revealed significant degrading activity in the 100,000 X g supernatant, but little activity in the 100,000 X g pellet. A purified lymphocyte preparation did not bind insulin and contained little insulin-degrading activity.

摘要

外周血中的单核细胞具有胰岛素受体,在某些代谢性疾病如肥胖症中,这些受体的数量或结合亲和力会发生改变。具有特异性结合胰岛素能力的细胞是单核细胞,而非淋巴细胞。此外,这种结合似乎反映了肝脏、肌肉和脂肪等胰岛素靶组织上的受体状态。由于肝脏、肌肉和脂肪也会降解胰岛素,因此对正常志愿者血液中的单核细胞进行了胰岛素降解活性检测。将完整细胞与¹²⁵I胰岛素一起孵育,通过三氯乙酸沉淀技术测量降解的胰岛素量。当细胞数量增加和孵育时间延长时,胰岛素降解活性增加。总胰岛素结合情况也类似。在4℃或15℃时,几乎看不到降解。胰岛素降解活性的米氏常数为7.03×10⁻⁸M。匀浆单核细胞降解的胰岛素比完整细胞多两到五倍,并且也表现出细胞浓度、时间和温度依赖性降解。匀浆单核细胞降解的米氏常数为2.2×10⁻⁸M。亚细胞分级分离显示,在100,000×g上清液中有显著的降解活性,但在100,000×g沉淀中活性很小。纯化的淋巴细胞制剂不结合胰岛素,且胰岛素降解活性很低。

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