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白细胞动力学研究。13. 可的松诱导粒细胞增多机制的非稳态动力学评估。

Leukokinetic studies. 13. A non-steady-state kinetic evaluation of the mechanism of cortisone-induced granulocytosis.

作者信息

Bishop C R, Athens J W, Boggs D R, Warner H R, Cartwright G E, Wintrobe M M

出版信息

J Clin Invest. 1968 Feb;47(2):249-60. doi: 10.1172/JCI105721.

Abstract

The mechanism by which adrenocortical steroids induce granulocytosis in man has been investigated using granulocytes labeled with radioactive diisopropylfluorophosphate. After an intravenous injection of 200 mg of cortisol was given to five normal subjects, the mean value for the total blood granulocyte pool increased from 79 to 138 x 10(7) cells per kg of body weight and reflected an increase in the size of both the circulating granulocyte pool and the marginal granulocyte pool. When granulocytes in the circulation were labeled with diisopropylfluorophosphate and granulocytosis was induced later by the intravenous administration of cortisol, the rate of decline of granulocyte specific activity was increased, indicating that the blood pool was being diluted at an accelerated rate by unlabeled cells entering from the bone marrow. The rate of egress of granulocytes from the blood pool to an inflammatory exudate was studied by the "skin window" technique. After the administration of cortisol, there was a mean reduction in the cellularity of induced inflammatory exudates of 75%. However, this reduction in cellularity varied considerably from subject to subject (45-98%). From these studies we can infer that steroids induce an absolute granulocytosis by decreasing the rate of egress of cells from the total blood granulocyte pool as well as by increasing the influx of cells from the bone marrow. By model simulation studies of the non-steady state induced by cortisol injection, it has been possible to quantitate these rate changes. In the present studies cortisol injection resulted in a mean decrease in blood granulocyte egress of 74% (1-99%) and a mean increase in cell inflow of 450% (300-750%).

摘要

利用放射性二异丙基氟磷酸标记的粒细胞,对肾上腺皮质类固醇在人体内诱导粒细胞增多的机制进行了研究。给5名正常受试者静脉注射200mg皮质醇后,每千克体重的全血粒细胞池平均值从79×10⁷个细胞增加到138×10⁷个细胞,这反映了循环粒细胞池和边缘粒细胞池的大小均有所增加。当用二异丙基氟磷酸标记循环中的粒细胞,随后通过静脉注射皮质醇诱导粒细胞增多时,粒细胞比活性的下降速率加快,这表明从骨髓进入的未标记细胞正在加速稀释血池。通过“皮肤窗”技术研究了粒细胞从血池进入炎性渗出液的逸出速率。给予皮质醇后,诱导的炎性渗出液中的细胞数平均减少了75%。然而,细胞数的减少在不同受试者之间差异很大(45%-98%)。从这些研究中我们可以推断,类固醇通过降低细胞从全血粒细胞池的逸出速率以及增加细胞从骨髓的流入量来诱导绝对的粒细胞增多。通过对皮质醇注射诱导的非稳态进行模型模拟研究,有可能对这些速率变化进行定量。在本研究中,皮质醇注射导致血粒细胞逸出平均减少74%(1%-99%),细胞流入平均增加450%(300%-750%)。

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