Institute for Cardiovascular and Metabolic Research, and.
School of Biological Sciences, University of Reading, Reading, United Kingdom.
Blood. 2021 Oct 21;138(16):1481-1489. doi: 10.1182/blood.2021011871.
A subset of patients with coronavirus disease 2019 (COVID-19) become critically ill, suffering from severe respiratory problems and also increased rates of thrombosis. The causes of thrombosis in severely ill patients with COVID-19 are still emerging, but the coincidence of critical illness with the timing of the onset of adaptive immunity could implicate an excessive immune response. We hypothesized that platelets might be susceptible to activation by anti-severe acute respiratory syndrome coronavirus 2 (anti-SARS-CoV-2) antibodies and might contribute to thrombosis. We found that immune complexes containing recombinant SARS-CoV-2 spike protein and anti-spike immunoglobulin G enhanced platelet-mediated thrombosis on von Willebrand factor in vitro, but only when the glycosylation state of the Fc domain was modified to correspond with the aberrant glycosylation previously identified in patients with severe COVID-19. Furthermore, we found that activation was dependent on FcγRIIA, and we provide in vitro evidence that this pathogenic platelet activation can be counteracted by the therapeutic small molecules R406 (fostamatinib) and ibrutinib, which inhibit tyrosine kinases Syk and Btk, respectively, or by the P2Y12 antagonist cangrelor.
一组新型冠状病毒病 2019(COVID-19)患者病情严重,出现严重呼吸问题,并伴有更高的血栓形成率。COVID-19 重症患者血栓形成的原因仍在不断出现,但重症与适应性免疫开始时间的巧合可能暗示过度的免疫反应。我们假设血小板可能容易被抗严重急性呼吸综合征冠状病毒 2(抗-SARS-CoV-2)抗体激活,并可能导致血栓形成。我们发现,含有重组 SARS-CoV-2 刺突蛋白和抗刺突免疫球蛋白 G 的免疫复合物在体外增强了血小板介导的血管性血友病因子依赖性血栓形成,但只有当 Fc 结构域的糖基化状态被修饰为与先前在 COVID-19 重症患者中发现的异常糖基化相匹配时才会发生这种情况。此外,我们发现这种激活依赖于 FcγRIIA,并且我们提供了体外证据表明,这种致病的血小板激活可以通过治疗性小分子 R406(福他替尼)和 ibrutinib 来拮抗,它们分别抑制酪氨酸激酶 Syk 和 Btk,或通过 P2Y12 拮抗剂坎格雷洛。
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