Identification of a Novel Splice Variant Isoform of TREM-1 in Human Neutrophil Granules.

IF 0.7 4区 化学 Q4 CHEMISTRY, ANALYTICAL
Lc Gc North America Pub Date : 2015-12-15 Epub Date: 2015-11-11 DOI:10.4049/jimmunol.1402713
Sankar Baruah, Kathy Keck, Michelle Vrenios, Marshall R Pope, Merideth Pearl, Kevin Doerschug, Julia Klesney-Tait
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引用次数: 0

Abstract

Triggering receptor expressed on myeloid cells-1 (TREM-1) is critical for inflammatory signal amplification. Humans have two forms of TREM-1: a membrane receptor, associated with the adaptor DAP12, and a soluble receptor detected at times of infection. The membrane receptor isoform acts synergistically with the TLR pathway to promote cytokine secretion and neutrophil migration, whereas the soluble receptor functions as a counterregulatory molecule. In multiple models of sepsis, exogenous administration of soluble forms of TREM-1 attenuates inflammation and markedly improves survival. Despite intense interest in soluble TREM-1, both as a clinical predictor of survival and as a therapeutic tool, the origin of native soluble TREM-1 remains controversial. Using human neutrophils, we identified a 15-kDa TREM-1 isoform in primary (azurophilic) and secondary (specific) granules. Mass spectrometric analysis, ELISA, and immunoblot confirm that the 15-kDa protein is a novel splice variant form of TREM-1 (TREM-1sv). Neutrophil stimulation with Pseudomonas aeruginosa, LPS, or PAM(3)Cys4 resulted in degranulation and release of TREM-1sv. The addition of exogenous TREM-1sv inhibited TREM-1 receptor-mediated proinflammatory cytokine production. Thus, these data reveal that TREM-1 isoforms simultaneously activate and inhibit inflammation via the canonical membrane TREM-1 molecule and this newly discovered granular isoform, TREM-1sv.

人中性粒细胞颗粒中 TREM-1 的一种新型剪接变异异构体的鉴定
髓系细胞上表达的触发受体-1(TREM-1)对炎症信号的放大至关重要。人类有两种形式的 TREM-1:一种是与适配体 DAP12 相关的膜受体,另一种是在感染时检测到的可溶性受体。膜受体异构体与 TLR 通路协同作用,促进细胞因子分泌和中性粒细胞迁移,而可溶性受体则作为反调节分子发挥作用。在多种败血症模型中,外源性给予可溶性 TREM-1 可减轻炎症反应并显著提高存活率。尽管人们对可溶性 TREM-1 作为临床生存预测指标和治疗工具产生了浓厚的兴趣,但本地可溶性 TREM-1 的来源仍存在争议。我们利用人体中性粒细胞,在原发性(嗜氮性)和继发性(特异性)颗粒中发现了一种 15 kDa 的 TREM-1 异构体。质谱分析、酶联免疫吸附试验和免疫印迹证实,这种 15 kDa 蛋白是 TREM-1 的一种新型剪接变异形式(TREM-1sv)。中性粒细胞受到铜绿假单胞菌、LPS 或 PAM(3)Cys4 的刺激后会脱颗粒并释放 TREM-1sv。添加外源性 TREM-1sv 可抑制 TREM-1 受体介导的促炎细胞因子的产生。因此,这些数据揭示了 TREM-1 异构体通过典型膜 TREM-1 分子和新发现的颗粒异构体 TREM-1sv 同时激活和抑制炎症。
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来源期刊
Lc Gc North America
Lc Gc North America 化学-分析化学
CiteScore
1.00
自引率
55.60%
发文量
0
审稿时长
2 months
期刊介绍: Founded in 1983, LCGC is the leading provider of digital and print content to the separation science market, enhancing the productivity, efficiency, and the overall value of separation techniques globally. Founded in 1983, LCGC is the leading provider of digital and print content to the separation science market, enhancing the productivity, efficiency, and the overall value of separation techniques globally. With our commitment to editorial excellence we have pioneered innovation across a broad portfolio of digital and print platforms.
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