特应性皮炎患者血清金属蛋白酶- 1组织抑制剂水平升高,而金属蛋白酶- 3不升高

N. Katoh, S. Hirano, M. Suehiro, K. Ikenaga, H. Yasuno
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引用次数: 27

摘要

基质金属蛋白酶及其特异性抑制剂,组织金属蛋白酶抑制剂(TIMPs),有助于炎症诱导的组织破坏和随后的重塑,以维持组织稳态。由于这些酶及其抑制剂的产生受促炎细胞因子和生长因子等介质的调节,在几种炎症性疾病患者中已记录到血清TIMPs和/或MMPs水平升高。在这项研究中,我们通过ELISA检测40例AD患者和20例对照者血清中TIMP‐1和MMP‐3的水平,研究了TIMP和MMPs在AD发病机制中的作用。AD患者在加重状态下的血清TIMP‐1水平明显高于非特应性受试者,而血清MMP‐3水平在他们之间无显著差异。结果显示,AD患者TIMP‐1/MMP‐3比值显著升高。常规治疗后,AD患者血清TIMP‐1水平显著降低。TIMP‐1水平升高的AD患者外周血嗜酸性粒细胞计数、血清IgE和乳酸脱氢酶水平、出疹评分和出疹面积均显著高于正常值的患者。此外,TIMP‐1水平升高的患者的慢性皮疹点(如地衣变和瘙痒)明显高于TIMP‐1水平正常的患者,而急性病变点(如渗出/微泡和水肿)在这两组之间没有差异。血清TIMP‐1水平可能是评估AD长期疾病活动性的有用指标。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Increased levels of serum tissue inhibitor of metalloproteinase‐1 but not metalloproteinase‐3 in atopic dermatitis
Matrix metalloproteinases and their specific inhibitors, tissue inhibitors of metalloproteinases (TIMPs), contribute to inflammation‐induced tissue destruction and subsequent remodeling for maintenance of tissue homeostasis. Since the production of these enzymes and their inhibitors is regulated by mediators such as proinflammatory cytokines and growth factors, elevated levels of serum TIMPs and/or MMPs have been documented in patients with several inflammatory disorders. In this study, we examined the role of TIMPs and MMPs in the pathogenesis of atopic dermatitis (AD) by evaluating the serum levels of TIMP‐1 and MMP‐3 in 40 patients with AD and 20 control subjects by ELISA. The serum TIMP‐1 levels were significantly higher in AD patients in exacerbation status than in nonatopic subjects, whereas serum MMP‐3 levels were not significantly different between them. As a result, AD patients revealed significantly elevated TIMP‐1/MMP‐3 ratios. The levels of serum TIMP‐1 were significantly reduced in AD patients following conventional treatments. Significantly higher values of peripheral eosinophil counts, serum levels of IgE and lactate dehydrogenase, eruption score, and eruption area were noted in the AD patients with elevated TIMP‐1 levels when compared with those with normal values. Moreover, the points of chronic eruptions such as lichenification and prurigo were significantly higher in the patients with elevated TIMP‐1 levels than those with normal TIMP‐1, while those of acute lesions such as oozy/microvesicles and oedema were not different between these groups. Serum TIMP‐1 level may be a useful marker to estimate the long‐term disease activity of AD.
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