Centre for Rheumatology and Connective Tissue Diseases, UCL Medical School, Royal Free Campus, Rowland Hill Street, London, NW3 2PF, UK.
Arthritis Res Ther. 2010;12(2):R69. doi: 10.1186/ar2986. Epub 2010 Apr 15.
Vasculopathy, including altered vasoreactivity and abnormal large vessel biomechanics, is a hallmark of systemic sclerosis (SSc). However, the pathogenic link with other aspects of the disease is less clear. To assess the potential role of transforming growth factor beta (TGF-beta) overactivity in driving these cardiovascular abnormalities, we studied a novel transgenic mouse model characterized by ligand-dependent activation of TGF-beta signaling in fibroblasts.
The transgenic mouse strain Tbeta RIIDeltak-fib is characterized by balanced ligand-dependent upregulation of TGF-beta signaling. Aortic and cardiac tissues were examined with histologic, biochemical, and isolated organ bath studies. Vascular and perivascular architecture was examined by hematoxylin and eosin (H&E) and special stains including immunostaining for TGF-beta1 and phospho-Smad2/3 (pSmad2/3). Confirmatory aortic smooth muscle cell proliferation, phenotype, and functional assays, including signaling responses to exogenous TGF-beta and endothelin-1, were performed. Aortic ring contractile responses to direct and receptor-mediated stimulation were assessed.
Aortic ring contractility and relaxation were diminished compared with wild-type controls, and this was associated with aortic adventitial fibrosis confirmed histologically and with Sircol assay. TGF-beta1 and pSmad 2/3 expression was increased in the adventitia and smooth muscle layer of the aorta. Aortic smooth muscle cells from transgenic animals showed significant upregulation of TGF-beta- responsive genes important for cytoskeletal function, such as transgelin and smoothelin, which were then resistant to further stimulation with exogenous TGF-beta1. These cells promoted significantly more contraction of free floating type I collagen lattices when compared with the wild-type, but were again resistant to exogenous TGF-beta1 stimulation. Aortic ring responses to receptor-mediated contraction were reduced in the transgenic animals. Specifically, bosentan reduced endothelin-mediated contraction in wild-type animals, but had no effect in transgenic animals, and endothelin axis gene expression was altered in transgenic animals. Transgenic mice developed cardiac fibrosis.
The histologic, biochemical, and functional phenotype of this transgenic mouse model of scleroderma offers insight into the altered biomechanical properties previously reported for large elastic arteries in human SSc and suggests a role for perturbed TGF-beta and endothelin activity in this process.
血管病变,包括血管反应性改变和大血管生物力学异常,是系统性硬化症(SSc)的一个标志。然而,与疾病其他方面的致病联系尚不清楚。为了评估转化生长因子β(TGF-β)过度活跃在驱动这些心血管异常中的潜在作用,我们研究了一种新型转基因小鼠模型,其特征是成纤维细胞中配体依赖性 TGF-β信号转导的激活。
TβRIIDeltak-fib 转基因小鼠品系的特征是配体依赖性 TGF-β信号转导的平衡上调。通过组织学、生化和离体器官浴研究检查主动脉和心脏组织。通过苏木精和伊红(H&E)和特殊染色(包括 TGF-β1 和磷酸化 Smad2/3(pSmad2/3)免疫染色)检查血管和血管周围结构。进行了确认的主动脉平滑肌细胞增殖、表型和功能测定,包括对外源性 TGF-β和内皮素-1的信号反应。评估了直接和受体介导刺激对主动脉环收缩反应的影响。
与野生型对照相比,主动脉环的收缩性和弛豫性降低,并且通过组织学和 Sircol 测定证实了主动脉外膜纤维化。TGF-β1 和 pSmad2/3 的表达在主动脉的外膜和平滑肌层中增加。来自转基因动物的主动脉平滑肌细胞显示出对细胞骨架功能重要的 TGF-β 反应基因的显著上调,例如转凝胶蛋白和 smoothelin,然后对进一步的外源性 TGF-β1 刺激具有抗性。与野生型相比,这些细胞可显著促进游离漂浮 I 型胶原格子的收缩,但对外源性 TGF-β1 刺激无反应。转基因动物的主动脉环对受体介导的收缩的反应降低。具体而言,波生坦降低了野生型动物内皮素介导的收缩,但对转基因动物没有影响,并且转基因动物的内皮素轴基因表达发生了改变。转基因小鼠发生了心脏纤维化。
这种硬皮病转基因小鼠模型的组织学、生化和功能表型提供了对先前报道的人类 SSc 大弹性动脉改变的生物力学特性的深入了解,并表明 TGF-β 和内皮素活性紊乱在该过程中起作用。
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