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外周血单核细胞衍生趋化因子阻断可预防鼠输血相关性急性肺损伤(TRALI)。

Peripheral blood monocyte-derived chemokine blockade prevents murine transfusion-related acute lung injury (TRALI).

机构信息

Toronto Platelet Immunobiology Group, Toronto, ON, Canada; Keenan Center for Biomedical Research, St. Michael's Hospital, Toronto, ON, Canada; Canadian Blood Services, Toronto, ON, Canada; and.

Toronto Platelet Immunobiology Group, Toronto, ON, Canada; Keenan Center for Biomedical Research, St. Michael's Hospital, Toronto, ON, Canada;

出版信息

Blood. 2014 May 29;123(22):3496-503. doi: 10.1182/blood-2013-11-536755. Epub 2014 Mar 17.

DOI:10.1182/blood-2013-11-536755
PMID:24637362
Abstract

Transfusion-related acute lung injury (TRALI) is the leading cause of transfusion-related mortality and can occur with any type of transfusion. TRALI is thought to be primarily mediated by donor antibodies activating recipient neutrophils resulting in pulmonary endothelial damage. Nonetheless, details regarding the interactions between donor antibodies and recipient factors are unknown. A murine antibody-mediated TRALI model was used to elucidate the roles of the F(ab')2 and Fc regions of a TRALI-inducing immunoglobulin G anti-major histocompatibility complex (MHC) class I antibody (34.1.2s). Compared with intact antibody, F(ab')2 fragments significantly increased serum levels of the neutrophil chemoattractant macrophage inflammatory protein 2 (MIP-2); however, pulmonary neutrophil levels were only moderately increased, and no pulmonary edema or mortality occurred. Fc fragments did not modulate any of these parameters. TRALI induction by intact antibody was completely abrogated by in vivo peripheral blood monocyte depletion by gadolinium chloride (GdCl3) or chemokine blockade with a MIP-2 receptor antagonist but was restored upon repletion with purified monocytes. The results suggest a two-step process for antibody-mediated TRALI induction: the first step involves antibody binding its cognate antigen on blood monocytes, which generates MIP-2 chemokine production that is correlated with pulmonary neutrophil recruitment; the second step occurs when antibody-coated monocytes increase Fc-dependent lung damage.

摘要

输血相关性急性肺损伤(TRALI)是输血相关死亡的主要原因,可发生于任何类型的输血。TRALI 被认为主要是由供体抗体激活受体中性粒细胞导致肺内皮损伤介导的。尽管如此,关于供体抗体和受体因素之间相互作用的细节尚不清楚。使用鼠抗体介导的 TRALI 模型阐明了诱导 TRALI 的免疫球蛋白 G 抗主要组织相容性复合物(MHC)I 类抗体(34.1.2s)的 F(ab')2 和 Fc 区域的作用。与完整抗体相比,F(ab')2 片段显著增加了中性粒细胞趋化因子巨噬细胞炎症蛋白 2(MIP-2)的血清水平;然而,肺中性粒细胞水平仅适度增加,并且没有发生肺水肿或死亡。Fc 片段没有调节这些参数中的任何一个。通过用钆氯化物(GdCl3)耗尽外周血单核细胞或用 MIP-2 受体拮抗剂阻断趋化因子来完全消除完整抗体诱导的 TRALI,但是在用纯化的单核细胞补充后恢复。结果表明抗体介导的 TRALI 诱导是一个两步过程:第一步涉及抗体与其在血液单核细胞上的同源抗原结合,产生与肺中性粒细胞募集相关的 MIP-2 趋化因子;第二步发生在抗体包被的单核细胞增加 Fc 依赖性肺损伤时。

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