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Treatment with DNAse I fosters binding to nec PBMC of CRP.

机译:DNAse I的治疗促进了与CRP的新PBMC的结合。

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摘要

CRP is an important inflammatory marker, however, CRP levels are relatively low in patients with SLE. In addition patients with SLE often display low activities and serum levels for DNase I and complement, respectively. Here we show that DNase I treatment of nec PBMC increased their binding of CRP. Consequently, reduced DNase I activity in patients with SLE may contribute to the impaired opsonisation by CRP of dead cells, exacerbating the clearance defect in SLE of apo and nec cells.
机译:CRP是重要的炎症标志物,但是SLE患者的CRP水平相对较低。此外,SLE患者经常表现出较低的DNase I和补体活性和血清水平。在这里,我们显示DNase I对新的PBMC的治疗增加了它们对CRP的结合。因此,SLE患者的DNase I活性降低可能会导致死细胞CRP的调理作用受损,加剧apo和nec细胞SLE的清除缺陷。

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