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肾上腺素能飙升与全身性毛细血管渗漏综合征(克拉克森病)的急性发作有关。

Adrenomedullin surges are linked to acute episodes of the systemic capillary leak syndrome (Clarkson disease).

机构信息

Molecular Signal Transduction Section, Laboratory of Allergic Diseases, St. Paul, Minnesota, USA.

Mast Cell Biology Section, Laboratory of Allergic Diseases, St. Paul, Minnesota, USA.

出版信息

J Leukoc Biol. 2018 Apr;103(4):749-759. doi: 10.1002/JLB.5A0817-324R. Epub 2018 Jan 23.

Abstract

BACKGROUND

Systemic Capillary Leak Syndrome (SCLS) is an extremely rare and life-threatening vascular disorder of unknown etiology. SCLS is characterized by abrupt and transient episodes of hypotensive shock and edema due to plasma leakage into peripheral tissues. The disorder has garnered attention recently because its initial presentation resembles more common vascular disorders including systemic anaphylaxis, sepsis, and acute infections with the Ebola/Marburg family of filoviruses. Although approximately 70-85% of patients with SCLS have a concurrent monoclonal gammopathy of unknown significance (MGUS), any contribution of the paraprotein to acute flares is unknown.

PROCEDURE

To identify circulating factors that might trigger acute SCLS crises, we profiled transcriptomes of paired peripheral blood mononuclear cell fractions obtained from patients during acute attacks and convalescent intervals by microarray.

RESULTS

This study uncovered 61 genes that were significantly up- or downregulated more than 2.5-fold in acute samples relative to respective baselines. One of the most upregulated genes was ADM, which encodes the vasoactive peptide adrenomedullin. A stable ADM protein surrogate (pro-ADM) was markedly elevated in SCLS acute sera compared to remission samples or sera from healthy controls. Monocytes and endothelial cells (ECs) from SCLS subjects expressed significantly more ADM in response to proinflammatory stimuli compared to healthy control cells. Application of ADM to ECs elicited protective effects on vascular barrier function, suggesting a feedback protective mechanism in SCLS.

CONCLUSIONS

Since ADM has established hypotensive effects, differentiating between these dual actions of ADM is crucial for therapeutic applications aimed at more common diseases associated with increased ADM levels.

摘要

背景

全身性毛细血管渗漏综合征(SCLS)是一种极其罕见且危及生命的血管疾病,病因不明。SCLS 的特征是由于血浆渗漏到外周组织中而导致突发性和短暂性低血压休克和水肿。该疾病最近受到关注,因为其初始表现类似于更常见的血管疾病,包括全身性过敏反应、败血症和急性感染埃博拉/马尔堡病毒科的丝状病毒。尽管大约 70-85%的 SCLS 患者伴有意义未明的单克隆丙种球蛋白血症(MGUS),但尚不清楚该副蛋白对急性发作的贡献。

程序

为了确定可能引发急性 SCLS 危象的循环因子,我们通过微阵列分析了患者在急性发作和恢复期采集的配对外周血单个核细胞分数的转录组。

结果

本研究发现 61 个基因在急性样本中相对于各自的基线显著上调或下调超过 2.5 倍。上调最明显的基因之一是编码血管活性肽肾上腺髓质素(adrenomedullin)的 ADM。SCLS 急性血清中的 ADM 稳定蛋白替代物(pro-ADM)明显高于缓解样本或健康对照者的血清。与健康对照细胞相比,SCLS 患者的单核细胞和内皮细胞(EC)在受到促炎刺激时表达的 ADM 明显增加。ADM 应用于 EC 可对血管屏障功能产生保护作用,提示 SCLS 中存在反馈保护机制。

结论

由于 ADM 具有降低血压的作用,因此区分 ADM 的这两种作用对于针对与 ADM 水平升高相关的更常见疾病的治疗应用至关重要。

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