Idiopathic multicentric Castleman disease - TAFRO results in high levels of mTOR activator SVEP1, tissue factor, and endotheliopathy

Blood Vessels, Thrombosis & Hemostasis Pub Date : 2024-04-03 DOI:10.1016/j.bvth.2024.100006

Chen Lossos , Jenna Brown , Sara Sheikhbahaei , Anne Hubben , Sharon C. Liu , Keith R. McCrae , Shruti Chaturvedi , Rakhi P. Naik , Ivo M.B. Francischetti

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Abstract

Idiopathic multicentric Castleman disease (iMCD) is an inflammatory disease associated with a cytokine storm, activation of the PI3K/AKT/mTOR pathway, coagulopathy, and increased risk of thrombosis. The mechanisms underlying these pathologic processes remain elusive. We studied novel markers of mTOR activation and thrombosis in 1 patient with typical features of iMCD with TAFRO (thrombocytopenia, anasarca, fevers, reticulin myelofibrosis, and organomegaly) syndrome (iMCD-TAFRO). Plasma levels of SVEP1 (Sushi, von Willebrand factor type A, epidermal growth factor, and pentraxin domain–containing 1 protein), a newly identified mTOR activator associated with cardiovascular diseases and dementia, in addition to cytokines, chemokines and components of the coagulation cascade and complement system were evaluated by enzyme-linked immunosorbent assay (ELISA) and arrays. Compared with healthy controls, a 15-fold increase in SVEP1 was observed. High levels of factor VIIa/antithrombin and microparticles expressing functional tissue factor (TF) were detected. The anticoagulants thrombomodulin and soluble endothelial protein C receptor were elevated, indicating shedding from endothelial cells. Plasminogen activator inhibitor 1 was increased, consistent with hypofibrinolysis, whereas high levels of C3b and C5a are in keeping with complement activation. Furthermore, markers of endothelial cell activation (e.g. von Willebrand factor, angiopoietin-2), cell adhesion molecules, and angiogenesis mediators were upregulated. SVEP1 emerges as a potential mechanism of mTOR activation in iMCD-TAFRO, while multiple pathways influence coagulopathy. Immunothrombosis emerges as a potential therapeutic target for iMCD.

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特发性多中心型 Castleman 病伴 TAFRO 综合征导致高水平的 mTOR 激活剂 SVEP1、组织因子、PAI-1 和内皮细胞病变

摘要特发性多中心卡斯特曼病（iMCD）是一种炎症性疾病，与细胞因子风暴、PI3K/AKT/mTOR 途径激活、凝血病变和血栓形成风险增加有关。这些病理过程的内在机制仍然难以捉摸。我们研究了一名具有 iMCD 伴 TAFRO（血小板减少、贫血、发热、网织红细胞骨髓纤维化和器官肥大）综合征（iMCD-TAFRO）典型特征的患者的 mTOR 激活和血栓形成的新标记物。除了细胞因子、趋化因子以及凝血级联和补体系统的成分外，还通过酶联免疫吸附试验（ELISA）和阵列评估了血浆中 SVEP1（Sushi、von Willebrand factor type A、表皮生长因子和含五肽结构域的 1 蛋白）的水平，SVEP1 是一种新发现的与心血管疾病和痴呆症有关的 mTOR 激活因子。与健康对照组相比，观察到 SVEP1 增加了 15 倍。检测到高水平的因子 VIIa/抗凝血酶和表达功能性组织因子（TF）的微颗粒。抗凝剂血栓调节蛋白和可溶性内皮蛋白 C 受体升高，表明内皮细胞脱落。纤溶酶原激活物抑制剂 1 增高，与纤溶不足相符，而高水平的 C3b 和 C5a 则与补体激活相符。此外，内皮细胞活化标志物（如 von Willebrand 因子、血管生成素-2）、细胞粘附分子和血管生成介质也出现了上调。SVEP1成为iMCD-TAFRO中mTOR激活的潜在机制，同时多种途径影响凝血病变。免疫血栓形成成为iMCD的潜在治疗靶点。

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Blood Vessels, Thrombosis & Hemostasis

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