转化生长因子-β与血管型(IV型)埃勒斯-当洛综合征中的炎症
Transforming growth factor-β and inflammation in vascular (type IV) Ehlers-Danlos syndrome.
作者信息
Morissette Rachel, Schoenhoff Florian, Xu Zhi, Shilane David A, Griswold Benjamin F, Chen Wuyan, Yang Jiandong, Zhu Jie, Fert-Bober Justyna, Sloper Leslie, Lehman Jason, Commins Natalie, Van Eyk Jennifer E, McDonnell Nazli B
机构信息
Laboratory of Clinical Investigation, National Institute on Aging, Baltimore, MD.
出版信息
Circ Cardiovasc Genet. 2014 Feb;7(1):80-8. doi: 10.1161/CIRCGENETICS.113.000280. Epub 2014 Jan 6.
BACKGROUND
Vascular Ehlers-Danlos syndrome (VEDS) causes reduced life expectancy because of arterial dissections/rupture and hollow organ rupture. Although the causative gene, COL3A1, was identified >20 years ago, there has been limited progress in understanding the disease mechanisms or identifying treatments.
METHODS AND RESULTS
We studied inflammatory and transforming growth factor-β (TGF-β) signaling biomarkers in plasma and from dermal fibroblasts from patients with VEDS. Analyses were done in terms of clinical disease severity, genotype-phenotype correlations, and body composition and fat deposition alterations. VEDS subjects had increased circulating TGF-β1, TGF-β2, monocyte chemotactic protein-1, C-reactive protein, intercellular adhesion molecule-1, vascular cell adhesion molecule-1, and leptin and decreased interleukin-8 versus controls. VEDS dermal fibroblasts secreted more TGF-β2, whereas downstream canonical/noncanonical TGF-β signaling was not different. Patients with COL3A1 exon skipping mutations had higher plasma intercellular adhesion molecule-1 and vascular cell adhesion molecule-1, and VEDS probands had abnormally high plasma C-reactive protein versus affected patients identified through family members before any disease manifestations. Patients with VEDS had higher mean platelet volumes, suggesting increased platelet turnover because of ongoing vascular damage, as well as increased regional truncal adiposity.
CONCLUSIONS
These findings suggest that VEDS is a systemic disease with a major inflammatory component. C-reactive protein is linked to disease state and may be a disease activity marker. No changes in downstream TGF-β signaling and increased platelet turnover suggest that chronic vascular damage may partially explain increased plasma TGF-β1. Finally, we found a novel role for dysregulated TGF-β2, as well as adipocyte dysfunction, as demonstrated through reduced interleukin-8 and elevated leptin in VEDS.
背景
血管型埃勒斯-当洛综合征(VEDS)因动脉夹层/破裂和中空器官破裂导致预期寿命缩短。尽管致病基因COL3A1在20多年前就已被确定,但在了解疾病机制或确定治疗方法方面进展有限。
方法与结果
我们研究了VEDS患者血浆和真皮成纤维细胞中的炎症和转化生长因子-β(TGF-β)信号生物标志物。根据临床疾病严重程度、基因型-表型相关性以及身体组成和脂肪沉积改变进行了分析。与对照组相比,VEDS患者循环中的TGF-β1、TGF-β2、单核细胞趋化蛋白-1、C反应蛋白、细胞间黏附分子-1、血管细胞黏附分子-1和瘦素增加,而白细胞介素-8减少。VEDS真皮成纤维细胞分泌更多的TGF-β2,而下游经典/非经典TGF-β信号无差异。COL3A1外显子跳跃突变患者的血浆细胞间黏附分子-1和血管细胞黏附分子-1较高,与在任何疾病表现出现之前通过家庭成员确定的受影响患者相比,VEDS先证者的血浆C反应蛋白异常高。VEDS患者的平均血小板体积较高,提示由于持续的血管损伤导致血小板周转率增加,以及躯干局部肥胖增加。
结论
这些发现表明VEDS是一种具有主要炎症成分的全身性疾病。C反应蛋白与疾病状态相关,可能是一种疾病活动标志物。下游TGF-β信号无变化以及血小板周转率增加表明慢性血管损伤可能部分解释了血浆TGF-β1升高。最后,我们发现失调的TGF-β2以及脂肪细胞功能障碍具有新的作用,这在VEDS中通过白细胞介素-8减少和瘦素升高得以证明。
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