视网膜血管病变伴脑白质脑病和全身表现(RVCL-S)患者体内的冯-威廉因子-ADAMTS-13 轴失衡。

Max Braune, Moritz Metelmann, Jonathan de Fallois, Christian Pfrepper, Alonso Barrantes-Freer, Grit Gesine Ruth Hiller, Susette Unger, Evelyn Seelow, Jan Halbritter, Johann Otto Pelz
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Renal biopsy of both RVCL-S patients and autoptic brain, renal, hepatic, and pulmonary specimen of one patient with RVCL-S were examined immunohistochemically in comparison to matched controls. In addition, cerebral methylome analysis was performed in the autoptic brain specimen calculating differentially methylated positions compared to controls.</p><p><strong>Results: </strong>While vWF-Ag and activity was strongly elevated, ADAMTS-13 activity was low in RVCL-S and further decreased over the course of the disease. Autoptic brain specimen showed signs of thromboinflammation in cerebral small vessels, and vWF-Ag staining was strongly positive in cerebral and renal small vessels in RVCL-S, while only a light to moderate vWF-Ag staining was found in controls. Cerebral methylome analysis yielded 115 differentially methylated CpGs (p < 0.05) in the deceased RVCL-S patient compared to the eight controls without brain pathology. 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摘要

背景:视网膜血管病变伴脑白质脑病和全身表现(RVCL-S)是一种超罕见的常染色体显性小血管疾病,由TREX1基因功能缺失变异引起。最近,血清中冯-威廉因子抗原(von Willebrand Factor Antigen,vWF-Ag)水平的升高指出了潜在的内皮病变,微血管缺血被认为是导致 RVCL-S 神经变性的原因之一。本研究旨在进一步阐明RVCL-S的内皮病变。方法:对两名经基因证实的RVCL-S患者的vWF-Ag和ADAMTS-13活性进行反复测量。与匹配的对照组相比,对两名RVCL-S患者的肾活检和一名RVCL-S患者的自体脑、肾、肝和肺标本进行了免疫组化检查。此外,还对自体脑标本进行了脑甲基组分析,计算出与对照组相比存在差异的甲基化位置:结果:RVCL-S患者的vWF-Ag和活性显著升高,而ADAMTS-13活性较低,并在病程中进一步降低。自体脑标本显示脑小血管有血栓炎症状,RVCL-S患者脑小血管和肾小管的vWF-Ag染色呈强阳性,而对照组仅有轻度至中度的vWF-Ag染色。脑甲基化组分析得出了 115 个不同甲基化的 CpGs(p 结论):这些发现表明,RVCL-S 患者体内的 vWF - ADAMTS-13 轴失衡,最终可能导致 vWF-Ag 在肾脏和脑小血管中积聚。vWF-Ag 水平升高可作为反映疾病活动的早期血清标志物。如果得到证实,未来的治疗方法可能会以抑制 vWF-Ag 或提高 ADAMTS-13 活性为目标。
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Imbalance of the von Willebrand Factor - ADAMTS-13 axis in patients with retinal vasculopathy with cerebral leukoencephalopathy and systemic manifestations (RVCL-S).

Background: Retinal vasculopathy with cerebral leukoencephalopathy and systemic manifestations (RVCL-S) is an ultra-rare, autosomal-dominant small vessel disease caused by loss-of-function variants in the gene TREX1. Recently, elevated serum levels of von Willebrand Factor Antigen (vWF-Ag) pointed to an underlying endotheliopathy, and microvascular ischemia was suggested to contribute to the neurodegeneration in RVCL-S. Aim of this study was to further elucidate the endotheliopathy in RVCL-S.

Methods: vWF-Ag and ADAMTS-13 activity were repeatedly measured in two patients with genetically confirmed RVCL-S. Renal biopsy of both RVCL-S patients and autoptic brain, renal, hepatic, and pulmonary specimen of one patient with RVCL-S were examined immunohistochemically in comparison to matched controls. In addition, cerebral methylome analysis was performed in the autoptic brain specimen calculating differentially methylated positions compared to controls.

Results: While vWF-Ag and activity was strongly elevated, ADAMTS-13 activity was low in RVCL-S and further decreased over the course of the disease. Autoptic brain specimen showed signs of thromboinflammation in cerebral small vessels, and vWF-Ag staining was strongly positive in cerebral and renal small vessels in RVCL-S, while only a light to moderate vWF-Ag staining was found in controls. Cerebral methylome analysis yielded 115 differentially methylated CpGs (p < 0.05) in the deceased RVCL-S patient compared to the eight controls without brain pathology. One of the hypomethylated genes coded for ADAMTS-13 (p = 0.00056).

Conclusions: These findings point to an imbalance of the vWF - ADAMTS-13 axis in patients with RVCL-S, that may finally lead to an accumulation of vWF-Ag in renal and cerebral small vessels. Elevated vWF-Ag levels may serve as an early serum marker reflecting disease activity. If confirmed, therapeutic approaches might aim at an inhibition of vWF-Ag or increase of ADAMTS-13 activity in the future.

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