The profile of adipokines associated with fibrosis and impaired microcirculation in systemic sclerosis

IF 2.5 4区 医学 Q3 MEDICINE, RESEARCH & EXPERIMENTAL
Anna Niemczyk, Anna Waśkiel-Burnat, Michał Zaremba, Joanna Czuwara, Lidia Rudnicka
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引用次数: 0

Abstract

Purpose

Adipokines belong to a group of molecules mostly produced by adipose tissue. Abnormalities in the secretion of several adipokines have already implicated to play a pathogenic role in systemic sclerosis (SSc). However, the possible role of numerous molecules still needs to be clarified. The aim of the study was to determine whether the altered level of selected circulating adipokines might correlate with the intensity of fibrosis and vasculopathy in the course of SSc.

Materials and methods

Serum concentrations of chemerin, adipsin, retinol-binding protein 4, apelin, visfatin, omentin-1, and vaspin were determined with ELISA in the sera of patients with SSc (n ​= ​55) and healthy controls (n ​= ​25).

Results

The serum concentration of adipsin (p ​= ​0.03) and visfatin (p ​= ​0.04) was significantly increased and the level of retinol-binding protein 4 (p ​= ​0.03) was decreased in diffuse compared to limited cutaneous SSc. Moreover, serum adipsin level correlated positively with the intensity of skin fibrosis measured with the modified Rodnan skin score (r ​= ​0.31, p ​= ​0.02) and was significantly higher in patients with pulmonary arterial hypertension than in those without the condition (p ​= ​0.03). The concentrations of adipsin (p ​= ​0.01) and visfatin (p ​= ​0.04) were significantly increased and the level of apelin (p ​= ​0.02) was decreased in patients with active digital ulcerations compared to individuals without this complication.

Conclusion

Adipsin may be considered a pivotal protein in the development of both fibrosis and impaired microcirculation. Its abnormal concentration reflects the intensity of skin thickening and the presence of pulmonary arterial hypertension. Adipsin, visfatin, and apelin are adipose tissue-derived molecules associated with digital vasculopathy.

系统性硬化症中脂肪因子与纤维化和微循环受损的关系
目的脂肪细胞因子属于一组主要由脂肪组织产生的分子。几种脂肪因子分泌的异常已经表明在系统性硬化症(SSc)中起着致病作用。然而,许多分子的可能作用仍有待澄清。该研究的目的是确定选定的循环脂肪因子水平的改变是否与SSc过程中的纤维化和血管病变的强度相关。材料与方法应用ELISA法测定慢性丙型肝炎患者血清中chemerin、adipsin、视黄醇结合蛋白4、apelin、visfatin、omentin-1和vaspin的血清浓度​=​55)和健康对照组(n​=​25)。结果血清组织蛋白酶(p​=​0.03)和visfatin(p​=​0.04)显著增加,视黄醇结合蛋白4(p​=​0.03)与有限的皮肤SSc相比在弥漫性中减少。此外,血清adipsin水平与用改良的Rodnan皮肤评分测量的皮肤纤维化强度呈正相关(r​=​0.31,p​=​0.02),并且在肺动脉高压患者中显著高于无肺动脉高压的患者(p​=​0.03)​=​0.01)和内脂素(p​=​0.04)显著升高,apelin(p​=​0.02)在具有活动性指溃疡的患者中与没有该并发症的个体相比降低。结论脂联素可能是纤维化和微循环障碍发生的关键蛋白。其异常浓度反映了皮肤增厚的强度和肺动脉高压的存在。脂肪蛋白酶、内脂蛋白和apelin是脂肪组织衍生的分子,与指血管病变有关。
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来源期刊
Advances in medical sciences
Advances in medical sciences 医学-医学:研究与实验
CiteScore
5.00
自引率
0.00%
发文量
53
审稿时长
25 days
期刊介绍: Advances in Medical Sciences is an international, peer-reviewed journal that welcomes original research articles and reviews on current advances in life sciences, preclinical and clinical medicine, and related disciplines. The Journal’s primary aim is to make every effort to contribute to progress in medical sciences. The strive is to bridge laboratory and clinical settings with cutting edge research findings and new developments. Advances in Medical Sciences publishes articles which bring novel insights into diagnostic and molecular imaging, offering essential prior knowledge for diagnosis and treatment indispensable in all areas of medical sciences. It also publishes articles on pathological sciences giving foundation knowledge on the overall study of human diseases. Through its publications Advances in Medical Sciences also stresses the importance of pharmaceutical sciences as a rapidly and ever expanding area of research on drug design, development, action and evaluation contributing significantly to a variety of scientific disciplines. The journal welcomes submissions from the following disciplines: General and internal medicine, Cancer research, Genetics, Endocrinology, Gastroenterology, Cardiology and Cardiovascular Medicine, Immunology and Allergy, Pathology and Forensic Medicine, Cell and molecular Biology, Haematology, Biochemistry, Clinical and Experimental Pathology.
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