甲氨蝶呤治疗前后银屑病皮损中角质细胞增殖、凋亡和皮肤炎症的研究:哪种变化对疾病的临床严重程度贡献更大?

A. A. Bary, A. Bary
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引用次数: 3

摘要

目的:银屑病的发病机制涉及t细胞介导的免疫应答、角化细胞增生和细胞凋亡抵抗。甲氨蝶呤是治疗针对这些变化的牛皮癣最可靠的方法之一。对甲氨蝶呤治疗前后这些变量的研究可能会回答这样一个问题:这些变量中哪一个对疾病的临床严重程度贡献更大,更有价值,更有针对性地治疗银屑病。患者与方法:选取寻常型银屑病患者50例,其中25例接受甲氨蝶呤治疗。治疗前后对银屑病皮损的皮肤活检进行组织学检查,以测量表皮厚度和皮肤炎症的分级。免疫染色检测Ki-67和p53,观察角质细胞增殖和凋亡情况。结果与疾病的临床严重程度相关,以银屑病面积和严重程度指数(PASI)评分进行评估。15例正常皮肤活检作为对照。结果:银屑病皮损组皮肤炎症、Ki-67%、p53%明显高于正常皮肤。这些变化与PASI评分显著相关。多元logistic回归模型显示Ki-67是影响临床严重程度的最显著变量。ki-67% 1个单位的变化可以解释PASI评分1.2个单位的变化,敏感性97%,特异性40%,临界值25%。甲氨蝶呤治疗后PASI评分、皮肤炎症、Ki-67%、P53%均显著降低。PASI评分下降百分比(81%)与Ki-67%(70%)之间无显著差异。结论:甲氨蝶呤治疗后,角化细胞增殖是影响银屑病临床严重程度的最显著变量,且该参数与PASI评分变化平行。角化细胞增殖可能被认为是银屑病所有其他病理和临床变化的刺激因素,应作为治疗的目标。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Study of Keratinocyte Proliferation, Apoptosis and Dermal Inflammation in Psoriatic Skin Lesions Before and After Methotrexate Therapy: Which Change Is Contributing More to Clinical Severity of the Disease?
Objective: The pathogenesis of psoriasis involves T-cell mediated immunologic response, keratinocytes hyperproliferation, and resistance to apoptosis. Methotrexate is one of the most reliable modalities in the treatment of psoriasis that target those changes. The study of those variables before and after methotrexate therapy may answer the question: Which of those variables contributes more to the clinical severity of the disease and is more valuable to be targeted in psoriasis treatment. Patients and Methods: A total of 50 cases of psoriasis vulgaris were included, 25 patients received methotrexate therapy. Skin biopsies of psoriatic skin lesions before and after treatment were examined histologically for measurement of epidermal thickness and grading of dermal inflammation. Immunostaining for Ki-67 and p53 was done for assessment of keratinocyte proliferation and apoptosis. Results were correlated with clinical severity of the disease, assessed by psoriatic area and severity index (PASI) score. 15 biopsies of normal skin were included as control. Results: Dermal inflammation, Ki-67%, and p53% were significantly higher in psoriatic skin lesion than in normal skin. Those changes were significantly correlated with PASI score. Multiple logistic regression models revealed that Ki-67 was the most significant variable contributing to clinical severity. One unit change in ki-67% can explain 1.2 unit changes in PASI score with 97% sensitivity, 40% specificity and 25% cut-off value. PASI score, dermal inflammation, Ki-67% and P53% were significantly reduced after methotrexate therapy. No significant difference was detected between the percent reduction in PASI score (81%) and that of Ki-67% (70%). Conclusion: Keratinocyte proliferation was the most significant variable contributing to the clinical severity of psoriasis and it was the single parameter that showed parallel changes to PASI score after methotrexate therapy. Keratinocyte proliferation may be considered as the stimulus that induces all other pathological and clinical changes in psoriasis and should be targeted by therapy.
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