硬皮病患者的内皮素-1水平:一项初步研究

ISRN Dermatology Pub Date : 2013-07-30 eCollection Date: 2013-01-01 DOI:10.1155/2013/125632
Emanuele Cozzani, Sanja Javor, Erika Laborai, Massimo Drosera, Aurora Parodi
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引用次数: 16

摘要

内皮素-1 (ET-1)是一种有效的内源性血管收缩剂,通过两种类型的ET-1受体(ET-A和ET-B)介导血管壁细胞增殖、纤维化和炎症。在我们的回顾性研究中,我们对18例伴有或不伴有数字溃疡(DUs)的系统性硬化症(SSc)患者的血清ET-1水平进行了评估,以观察ET-1水平、SSc的发展和ET-1拮抗剂(波生坦)治疗之间可能的相关性。在我们所有的患者中,ET-1水平均高于正常范围,并与疾病的严重程度相关。此外,我们还观察到,在没有DUs的患者中,ET-1水平较高,与新DUs的发展无关。总之,我们研究的患者中ET-1的水平与DUs的可能发展无关。波生坦治疗的DUs患者ET-1水平的降低证实了这种分子在治疗和预防指溃疡方面的功效。拮抗剂对ET-A受体的抑制可能激活相反的ET-B受体,具有众所周知的ET-1降解和降低ET-1血清水平的功能,这在我们的前期研究中得到了证实。
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Endothelin-1 levels in scleroderma patients: a pilot study.

Endothelin-1 (ET-1) is a potent endogenous vasoconstrictor, which mediates vascular wall cells proliferation, fibrosis, and inflammation through two types of ET-1 receptors (ET-A and ET-B). In our retrospective study the serum levels of ET-1 in 18 systemic sclerosis (SSc) patients with and without digital ulcers (DUs) were assessed to observe possible correlation between the levels of ET-1, the evolution of SSc, and the therapy with an ET-1 antagonist (bosentan). In all our patients, the levels of ET-1 were found higher than normal range and correlate with the severity of the disease. Furthermore we also observed that in patients without DUs the levels of ET-1 were higher and did not correlate with new DUs development. In conclusion, the levels of ET-1 in our studied patients do not correlate with the possible development of DUs. The reduction of ET-1 levels in DUs patients in therapy with bosentan confirms the efficacy of this molecule both for treatment and prevention of digital ulcers. The inhibition of ET-A receptor by its antagonist may activate the opposite ET-B receptors, with well-known function ET-1 degradation and reducing of ET-1 serum level as confirmed in our pilot study.

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