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体外血液透析膜相互作用后单核细胞和粒细胞上CD11b/CD18的调节

Modulation of CD11b/CD18 on monocytes and granulocytes following hemodialysis membrane interaction in vitro.

作者信息

Thylén P, Fernvik E, Lundahl J, Hed J, Jacobson S H

机构信息

Department of Internal Medicine, Karolinska Hospital, Stockholm, Sweden.

出版信息

Int J Artif Organs. 1996 Mar;19(3):156-63.

PMID:8675359
Abstract

We studied the generation of CD11b/CD18 mobilizing factors in serum after incubation with dialysis membrane fragments of different chemical composition. We also evaluated the relative importance of the alternative and classical pathways of the complement system in the generation of such factors. Monocytes and granulocytes from healthy blood donors were incubated in normal human serum (NHS) and in NHS that had been preincubated with Cuprophan (CU) membrane (NHS-CU), Hemophan (HE) (NHS-HE) or polysulfone (PS) (NHS-PS). NHS-CU caused the highest up-regulation of the CD11b/CD18 receptor on monocytes and granulocytes. The rank in capacity to mobilize CD11b/CD18 on granulocytes was CU > HE > PS (p < 0.001), CU > HE (p < 0.05) and HE > PS (p < 0.001). The rank in capacity to mobilize CD11b/CD18 on monocytes was CU > HE > PS (p < 0.001), CU > HE (p < 0.05) and HE > PS (p < 0.01). NHS-PS induced a lower up-regulation of CD11b/CD18 compared to NHS which indicates that serum factors with the ability to mobilize the CD11b/CD18 receptor on monocytes and granulocytes are deposited on or absorbed by PS. In order to study the relative contribution of the alternative and classical pathways of the complement system in the generation of CD11b/CD18 mobilizing factors in serum, three different serum preparations (1. both pathways intact. 2. only the alternative intact and 3. only the classical pathway intact) were used. The CU membrane activated the classical pathway to a larger extent than the PS membrane (p < 0.01). When only the alternative pathway was intact no difference in the generation of CD11b/CD18 mobilizing factors between the CU and PS membranes was observed. These studies show that CD11b/CD18 mobilizing serum factors are generated after incubation with CU membranes and that such factors are probably adsorbed by PS. The classical pathway of complement activation seems to contribute to the generation of CD11b/CD18 mobilizing factors in serum.

摘要

我们研究了不同化学成分的透析膜片段孵育后血清中CD11b/CD18动员因子的产生情况。我们还评估了补体系统替代途径和经典途径在这类因子产生过程中的相对重要性。将健康献血者的单核细胞和粒细胞分别置于正常人血清(NHS)以及预先与铜仿(CU)膜、血仿(HE)或聚砜(PS)膜孵育过的NHS(NHS-CU、NHS-HE或NHS-PS)中。NHS-CU导致单核细胞和粒细胞上CD11b/CD18受体的上调程度最高。在粒细胞上动员CD11b/CD18的能力排序为:CU>HE>PS(p<0.001),CU>HE(p<0.05),HE>PS(p<0.001)。在单核细胞上动员CD11b/CD18的能力排序为:CU>HE>PS(p<0.001),CU>HE(p<0.05),HE>PS(p<0.01)。与NHS相比,NHS-PS诱导的CD11b/CD18上调程度较低,这表明具有在单核细胞和粒细胞上动员CD11b/CD18受体能力的血清因子会沉积在PS上或被PS吸附。为了研究补体系统替代途径和经典途径在血清中CD11b/CD18动员因子产生过程中的相对贡献,使用了三种不同的血清制剂(1. 两条途径均完整;2. 仅替代途径完整;3. 仅经典途径完整)。CU膜比PS膜更能激活经典途径(p<0.01)。当仅替代途径完整时,未观察到CU膜和PS膜在CD11b/CD18动员因子产生方面的差异。这些研究表明,与CU膜孵育后会产生CD11b/CD18动员血清因子,且这类因子可能会被PS吸附。补体激活的经典途径似乎有助于血清中CD11b/CD18动员因子的产生。

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