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体外和体内地塞米松对人中性粒细胞功能的影响。

The effect of in vitro and in vivo dexamethasone on human neutrophil function.

作者信息

Lomas D A, Ip M, Chamba A, Stockley R A

机构信息

Lung Immunobiochemical Research Laboratory, General Hospital, Birmingham, U.K.

出版信息

Agents Actions. 1991 Jul;33(3-4):279-85. doi: 10.1007/BF01986574.

Abstract

There is a significant fall in PMN chemotaxis to the peptide FMLP in response to increasing concentrations of dexamethasone in vitro. The response fell in a dose related manner from a control value of 53.7 SE +/- 9.6 cells per high power field (cpf) to 47.3 SE +/- 8.1 at 10(-6) M (p less than 0.05) and 24.7 +/- 8.9 at 10(-3) M (p less than 0.025). A similar response was observed for the chemoattractants zymosan activated serum and the sol phase of purulent sputum. The effect was independent of protein synthesis or the period of incubation. Twelve milligrams of dexamethasone taken daily by 6 healthy volunteers resulted in a significant (p less than 0.025) reduction in the chemotactic response of PMN to 10(-8) M FMLP (from 29.5 +/- 1.55 to 13.7 +/- 1.8 cpf) which was apparent within 2 hours of taking the first dose. This effect was sustained for the three days on which dexamethasone was taken but returned to normal 7 days after the last dose had been administered. Dexamethasone therapy had no effect on unstimulated PMN superoxide anion production either in vitro or in vivo. The in vivo effect on neutrophil function occurred at mean serum dexamethasone concentrations of 1.26 (+/- 0.28) X 10(-7) M on day 1, 1.44 (+/- 0.15) X 10(-7) M on day 2 and 1.31 (+/- 0.13) X 10(-7) M on day 3. Thus we conclude that dexamethasone concentration which inhibit PMN chemotaxis in vivo are much lower than those required to exert the same effect in vitro.

摘要

在体外,随着地塞米松浓度的增加,中性粒细胞对肽FMLP的趋化性显著下降。反应以剂量相关的方式下降,从每高倍视野(cpf)53.7 SE±9.6个细胞的对照值降至10(-6) M时的47.3 SE±8.1(p<0.05)和10(-3) M时的24.7±8.9(p<0.025)。对于趋化剂酵母聚糖活化血清和脓性痰液的液相也观察到类似的反应。该效应与蛋白质合成或孵育时间无关。6名健康志愿者每日服用12毫克地塞米松导致中性粒细胞对10(-8) M FMLP的趋化反应显著降低(p<0.025)(从29.5±1.55降至13.7±1.8 cpf),在服用首剂后2小时内即可显现。该效应在地塞米松服用的三天内持续存在,但在最后一剂给药7天后恢复正常。地塞米松治疗在体外或体内对未刺激的中性粒细胞超氧化物阴离子产生均无影响。体内对中性粒细胞功能的影响发生在第1天平均血清地塞米松浓度为1.26(±0.28)×10(-7) M、第2天为1.44(±0.15)×10(-7) M和第3天为1.31(±0.13)×10(-7) M时。因此我们得出结论,体内抑制中性粒细胞趋化性的地塞米松浓度远低于在体外产生相同效应所需的浓度。

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