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刺激的单核细胞产物对中性粒细胞对C5a去精氨酸反应的启动作用。

The priming effects of the products of stimulated mononuclear cells on the response of neutrophils to C5a des arg.

作者信息

Crouch S, Fletcher J

机构信息

Medical Research Centre, City Hospital, Nottingham.

出版信息

Br J Haematol. 1991 Feb;77(2):158-64. doi: 10.1111/j.1365-2141.1991.tb07971.x.

Abstract

Certain recombinant human cytokines have been shown to enhance polymorphonuclear leucocyte (PMN) responses to subsequent stimulation. Mononuclear cells (MNC) from normal healthy individuals were stimulated for 5 h with 1 micrograms/ml bacterial lipopolysaccharide (LPS) in order to induce production and secretion of inflammatory cytokines into the surrounding medium. These mononuclear cell conditioned media (MNCM) were then used to prime PMN isolated from healthy volunteers. Preincubating the PMN with MNCM for 15 min at 4 degrees C followed by washing and warming to 37 degrees C caused a 344% increase (n = 26) in the rate of superoxide anion production in response to zymosan-activated serum (ZAS), a source of C5a des arg. This effect could not be reproduced with recombinant human forms of interleukin 1 beta (Il-1 beta) or granulocyte-macrophage-colony stimulating factor (GM-CSF), although, with the latter, there was some effect when the preincubation stage was carried out for 60 min at 37 degrees C. Only recombinant human tumour necrosis factor-alpha (rh-TNF-alpha) gave a similar PMN priming effect to that seen with MNCM. This effect could not be reversed by washing away either the MNCM or rh-TNF-alpha. The priming effect could be markedly reduced (74.8%, n = 6) by employing the use of polyclonal antibody to TNF-alpha in the preincubation step; assaying for TNF-alpha in these MNCMs showed that the degree of priming corresponded to the amount of TNF-alpha present. Rh-TNF-alpha alone appeared to have very little direct stimulatory effect on respiratory burst activity. The results show that TNF-alpha produced by LPS stimulated MNC after 5 h binds to a PMN surface receptor in the cold and warming of the cells to 37 degrees C allows for an immediate and dramatic response to ZAS stimulation. This suggests that TNF-alpha is the important cytokine upregulating PMN responses to other physiological mediators, including C5a des arg during the early phases of an inflammatory reaction.

摘要

某些重组人细胞因子已被证明可增强多形核白细胞(PMN)对后续刺激的反应。来自正常健康个体的单核细胞(MNC)用1微克/毫升细菌脂多糖(LPS)刺激5小时,以诱导炎症细胞因子产生并分泌到周围培养基中。然后将这些单核细胞条件培养基(MNCM)用于预处理从健康志愿者中分离出的PMN。在4℃下将PMN与MNCM预孵育15分钟,然后洗涤并升温至37℃,会使对酵母聚糖激活血清(ZAS,一种C5a去精氨酸的来源)的超氧阴离子产生速率增加344%(n = 26)。重组人白细胞介素1β(Il-1β)或粒细胞-巨噬细胞集落刺激因子(GM-CSF)的形式无法重现这种效果,不过,对于后者,当在37℃下预孵育阶段进行60分钟时会有一些效果。只有重组人肿瘤坏死因子-α(rh-TNF-α)产生了与MNCM类似的PMN预处理效果。通过洗去MNCM或rh-TNF-α都无法逆转这种效果。在预孵育步骤中使用抗TNF-α的多克隆抗体可使预处理效果显著降低(74.8%,n = 6);对这些MNCM中的TNF-α进行检测表明,预处理程度与存在的TNF-α量相对应。单独的rh-TNF-α似乎对呼吸爆发活性几乎没有直接刺激作用。结果表明,LPS刺激的MNC在5小时后产生的TNF-α在低温下与PMN表面受体结合,将细胞升温至37℃可使其对ZAS刺激立即产生显著反应。这表明TNF-α是在炎症反应早期上调PMN对其他生理介质(包括C5a去精氨酸)反应的重要细胞因子。

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