白癜风患者血清中 CXCL9 和 CXCL10 水平的差异表达及其与疾病严重程度和稳定性的相关性:横断面研究

Shayna Aulakh, Seema Goel, Loveleen Kaur, Samridhi Gulati, Maninder Kaur, D. Chopra, Rishu Sarangal, Jayati Batra
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引用次数: 0

摘要

白癜风是一种获得性色素脱失症,其发病机制难以捉摸,但已有多种理论提出。皮损周围自反应性 CD8+ T 细胞浸润的存在表明,异常免疫反应和自身免疫参与了白癜风的发病。最近的研究发现,IFN-γ-CXCL9/CXCL-10 轴是自身免疫反应的一个关键组成部分,它使白癜风的疾病活动持续存在。此外,该研究还旨在发现CXCL9和CXCL10水平与疾病严重程度和稳定性之间的相关性。次要目标包括比较节段型/非节段型白癜风和稳定期/进展期白癜风的水平,以及评估年龄和性别的影响。这项以医院为基础的横断面研究包括60名白癜风患者和30名年龄和性别匹配的对照组。采用酶联免疫吸附试验(ELISA)评估血清中CXCL9和CXCL10的水平。临床评估病例的白癜风类型(节段型或非节段型)、疾病严重程度(VASI评分)和疾病稳定性(VIDA评分)。统计分析包括 t 检验、卡方检验和相关系数。与对照组相比,白癜风患者的血清 CXCL9 和 CXCL10 均显著升高(p 值分别为 0.001* 和 0.001*),并与 VASI 评分(p 值分别为 0.001* 和 0.001*)和 VIDA 评分(p 值分别为 0.032* 和 0.001*)呈正相关。血清 CXCL10 在进展期白癜风中明显升高,而 CXCL9 则无明显趋势。节段性和非节段性白癜风之间没有明显差异。趋化因子CXCL9和CXCL10的表达明显增加,并与疾病的严重程度和不稳定性呈正相关,强调了它们在白癜风发病机制中的作用。进展期组的CXCL9和CXCL10值也高于稳定期组,这说明它们有可能成为血清生物标记物。与对照组相比,白癜风患者血清中的CXCL9和CXCL10均明显升高,可作为潜在的血清生物标志物用于评估疾病的活动性。自愿抽样技术导致进展期和稳定期白癜风组、节段型和非节段型白癜风组的患者人数不均等。趋化因子CXCL9和CXCL10的表达明显增加,并与疾病的严重程度和不稳定性呈正相关,强调了它们在白癜风发病机制中的作用。进展期组的数值也高于稳定期组,这推断出它们有可能成为血清生物标志物。
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Differential expression of serum CXCL9 and CXCL10 levels in vitiligo patients and their correlation with disease severity and stability: A cross-sectional study
Vitiligo is an acquired disorder of pigmentation with an elusive pathogenesis, though various theories have been proposed. The presence of peri-lesional autoreactive CD8+ T cell infiltrate suggests the involvement of abnormal immune responses and autoimmunity in vitiligo. Recent studies have identified the IFN-γ-CXCL9/CXCL-10 axis as a key component of the autoimmune response that perpetuates disease activity in vitiligo. The primary objective was to estimate serum CXCL9 and CXCL10 levels in vitiligo patients compared to age- and sex-matched controls. Additionally, the study aimed to find correlations between CXCL9 and CXCL10 levels and disease severity and stability. Secondary objectives included comparing levels in segmental/nonsegmental vitiligo and stable/progressive vitiligo and assessing the impact of age and gender. A hospital-based cross-sectional study included 60 vitiligo patients and 30 age- and sex-matched controls. Serum levels of CXCL9 and CXCL10 were assessed using Enzyme-linked immunosorbent assay (ELISA). Cases were clinically evaluated for the type of vitiligo (segmental or non-segmental), disease severity (VASI score), and disease stability (VIDA score). Statistical analysis included t-tests, chi-square tests, and correlation coefficients. P value less than 0.5 was taken as significant. Serum CXCL9 and CXCL10, both, were significantly raised in vitiligo patients as compared to controls (p-value = 0.001* & 0.001* respectively) and correlated positively with both VASI score (p-value = 0.001* & 0.001* respectively) and with VIDA score (p-value = 0.032* & 0.001* respectively). Serum CXCL10 showed significant elevation in progressive vitiligo, and CXCL9 exhibited a non-significant trend. No significant difference was observed between segmental and non-segmental vitiligo. Both chemokines positively correlated with disease severity and stability, while age and gender did not significantly impact chemokine levels. The expression of chemokines CXCL9 and CXCL10 is markedly increased and correlated positively with disease severity & instability, underscoring their mechanistic role in vitiligo pathogenesis. The values were also higher in the progressive group than in the stable group, inferring their conceivable potential as serum biomarkers. Both serum CXCL9 and CXCL10 were significantly elevated in vitiligo patients compared to controls and they can be used as potential serum biomarkers for assessing the disease activity. Small sample size of control population. The voluntary sampling technique led to an unequal number of patients in progressive and stable vitiligo groups, as well as in segmental and non-segmental groups. The current study did not include blister fluid analysis and the effect of therapy on the chemokine levels. The expression of chemokines CXCL9 and CXCL10 is markedly increased and correlates positively with disease severity and instability, underscoring their mechanistic role in vitiligo pathogenesis. The values were also higher in the progressive group than in the stable group, inferring their conceivable potential as serum biomarkers. *represents statistically significant results
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