组织因子
免疫学
抗磷脂综合征
促炎细胞因子
生物
狼疮抗凝剂
系统性红斑狼疮
凝结
抗体
医学
炎症
内科学
疾病
作者
Nadine Müller‐Calleja,Kristin Grunz,Thanh‐Son Nguyen,Jens Posma,Denise Pedrosa,Myriam Meineck,Anne Hollerbach,Johannes Braun,Sabine Muth,Hansjörg Schild,Kathrin Saar,Norbert Hübner,Sriram Krishnaswamy,Jennifer Royce,Luc Teyton,Niels A. W. Lemmermann,Julia Weinmann‐Menke,Karl J. Lackner,Wolfram Ruf
出处
期刊:Blood
[American Society of Hematology]
日期:2023-12-24
卷期号:143 (12): 1167-1180
被引量:2
标识
DOI:10.1182/blood.2023022276
摘要
Abstract Antiphospholipid antibodies (aPL) in primary or secondary antiphospholipid syndrome (APS) are a major cause for acquired thrombophilia, but specific interventions preventing autoimmune aPL development are an unmet clinical need. Although autoimmune aPL cross react with various coagulation regulatory proteins, lipid-reactive aPL, including those derived from patients with COVID-19, recognize the endolysosomal phospholipid lysobisphosphatidic acid presented by the cell surface–expressed endothelial protein C receptor. This specific recognition leads to complement-mediated activation of tissue factor (TF)–dependent proinflammatory signaling and thrombosis. Here, we show that specific inhibition of the TF coagulation initiation complex with nematode anticoagulant protein c2 (NAPc2) prevents the prothrombotic effects of aPL derived from patients with COVID-19 in mice and the aPL–induced proinflammatory and prothrombotic activation of monocytes. The induction of experimental APS is dependent on the nicotinamide adenine dinucleotide phosphate (NADPH) oxidase complex, and NAPc2 suppresses monocyte endosomal reactive oxygen species production requiring the TF cytoplasmic domain and interferon-α secretion from dendritic cells. Latent infection with murine cytomegalovirus causes TF cytoplasmic domain–dependent development of persistent aPL and circulating phospholipid-reactive B1 cells, which is prevented by short-term intervention with NAPc2 during acute viral infection. In addition, treatment of lupus prone MRL-lpr mice with NAPc2, but not with heparin, suppresses dendritic-cell activation in the spleen, aPL production and circulating phospholipid-reactive B1 cells, and attenuates lupus pathology. These data demonstrate a convergent TF-dependent mechanism of aPL development in latent viral infection and autoimmune disease and provide initial evidence that specific targeting of the TF initiation complex has therapeutic benefits beyond currently used clinical anticoagulant strategies.
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