Mechanical and Aerospace Engineering Department, Case Western Reserve University, Cleveland, Ohio, USA.
Department of Biomedical Engineering, University of Houston, Houston, Texas, USA.
Br J Haematol. 2023 May;201(3):552-563. doi: 10.1111/bjh.18616. Epub 2023 Jan 5.
Endothelial activation and sickle red blood cell (RBC) adhesion are central to the pathogenesis of sickle cell disease (SCD). Quantitatively, RBC-derived extracellular vesicles (REVs) are more abundant from SS RBCs compared with healthy RBCs (AA RBCs). Sickle RBC-derived REVs (SS REVs) are known to promote endothelial cell (EC) activation through cell signalling and transcriptional regulation at longer terms. However, the SS REV-mediated short-term non-transcriptional response of EC is unclear. Here, we examined the impact of SS REVs on acute microvascular EC activation and RBC adhesion at 2 h. Compared with AA REVs, SS REVs promoted human pulmonary microvascular ECs (HPMEC) activation indicated by increased von Willebrand factor (VWF) expression. Under microfluidic conditions, we found abnormal SS RBC adhesion to HPMECs exposed to SS REVs. This enhanced SS RBC adhesion was reduced by haeme binding protein haemopexin or VWF cleaving protease ADAMTS13 to a level similar to HPMECs treated with AA REVs. Consistent with these observations, haemin- or SS REV-induced microvascular stasis in SS mice with implanted dorsal skin-fold chambers that was inhibited by ADAMTS13. The adhesion induced by SS REVs was variable and was higher with SS RBCs from patients with increased markers of haemolysis (lactate dehydrogenase and reticulocyte count) or a concomitant clinical diagnosis of deep vein thrombosis. Our results emphasise the critical contribution made by REVs to the pathophysiology of SCD by triggering acute microvascular EC activation and abnormal RBC adhesion. These findings may help to better understand acute pathophysiological mechanism of SCD and thereby the development of new treatment strategies using VWF as a potential target.
内皮细胞激活和镰状红细胞(RBC)黏附是镰状细胞病(SCD)发病机制的核心。从定量上看,与健康的 RBC(AA RBC)相比,RBC 来源的细胞外囊泡(REV)在 SS RBC 中更为丰富。已知镰状 RBC 来源的 REV(SS REV)通过细胞信号转导和长期转录调控促进内皮细胞(EC)激活。然而,SS REV 介导的 EC 短期非转录反应尚不清楚。在这里,我们研究了 SS REV 对 2 小时内急性微血管 EC 激活和 RBC 黏附的影响。与 AA REV 相比,SS REV 促进人肺微血管内皮细胞(HPMEC)激活,表现为 von Willebrand 因子(VWF)表达增加。在微流控条件下,我们发现异常的 SS RBC 黏附到暴露于 SS REV 的 HPMEC 上。这种增强的 SS RBC 黏附通过血红素结合蛋白血红素结合蛋白或 VWF 切割蛋白酶 ADAMTS13 降低到与用 AA REV 处理的 HPMEC 相似的水平。与这些观察结果一致,血红素或 SS REV 诱导的 SS 小鼠背皮囊植入的微血管停滞,ADAMTS13 抑制了这种停滞。SS REV 诱导的黏附是可变的,并且在用增加的溶血标志物(乳酸脱氢酶和网织红细胞计数)或同时伴有深静脉血栓形成的临床诊断的 SS RBC 中更高。我们的研究结果强调了 REV 通过触发急性微血管 EC 激活和异常 RBC 黏附对 SCD 病理生理学的重要贡献。这些发现可能有助于更好地理解 SCD 的急性病理生理机制,并由此开发使用 VWF 作为潜在靶点的新治疗策略。