重庆医学
重慶醫學
중경의학
CHONGQING MEDICAL JOURNAL
2014年
31期
4225-4226,4229
,共3页
叶筱燕%戴永江%蒙秉新%曾慧明%丁艳
葉篠燕%戴永江%矇秉新%曾慧明%丁豔
협소연%대영강%몽병신%증혜명%정염
白癜风%白细胞介素 22%趋化因子
白癜風%白細胞介素 22%趨化因子
백전풍%백세포개소 22%추화인자
vitiligo%interleukin-22%Chemokine
目的:检测寻常型白癜风患者外周血清中趋化因子9(CXCL9)表达水平并探讨其临床意义。方法采用ELISA法检测35例寻常型白癜风患者(进展期20例,稳定期15例)和20例健康对照者血清 CXCL9及 IL‐22含量。比较 CXCL9、IL‐22在各组血清中含量的差异,分析 CXCL9、IL‐22与白瘫风患者年龄、病程及皮损面积的相关性。结果经统计学分析,进展期白癜风患者和稳定期白癜风患者血清 CXCL9、IL‐22含量明显高于对照组(P<0.05);进展期白癜风患者血清 CXCL9、IL‐22明显高于稳定期白癜风患者,差异有统计学意义(P<0.05)。结论 CXCL9、IL‐22可能参与了白癜风的发病过程。
目的:檢測尋常型白癜風患者外週血清中趨化因子9(CXCL9)錶達水平併探討其臨床意義。方法採用ELISA法檢測35例尋常型白癜風患者(進展期20例,穩定期15例)和20例健康對照者血清 CXCL9及 IL‐22含量。比較 CXCL9、IL‐22在各組血清中含量的差異,分析 CXCL9、IL‐22與白癱風患者年齡、病程及皮損麵積的相關性。結果經統計學分析,進展期白癜風患者和穩定期白癜風患者血清 CXCL9、IL‐22含量明顯高于對照組(P<0.05);進展期白癜風患者血清 CXCL9、IL‐22明顯高于穩定期白癜風患者,差異有統計學意義(P<0.05)。結論 CXCL9、IL‐22可能參與瞭白癜風的髮病過程。
목적:검측심상형백전풍환자외주혈청중추화인자9(CXCL9)표체수평병탐토기림상의의。방법채용ELISA법검측35례심상형백전풍환자(진전기20례,은정기15례)화20례건강대조자혈청 CXCL9급 IL‐22함량。비교 CXCL9、IL‐22재각조혈청중함량적차이,분석 CXCL9、IL‐22여백탄풍환자년령、병정급피손면적적상관성。결과경통계학분석,진전기백전풍환자화은정기백전풍환자혈청 CXCL9、IL‐22함량명현고우대조조(P<0.05);진전기백전풍환자혈청 CXCL9、IL‐22명현고우은정기백전풍환자,차이유통계학의의(P<0.05)。결론 CXCL9、IL‐22가능삼여료백전풍적발병과정。
Objective To detect the expression level of CXCL9 and IL‐22 in peripheral blood of patients with vitiligo vulgaris and explore its role in the pathogenesis of vitiligo vulgaris .Methods The level of CXCL9 and IL‐22 in peripheral blood from 35 vit‐iligo patients (20 active cases and 15 stable cases) and 20 normal controls were measured by enzyme linked immunosorbent assay . Then ,we compared the differences in different groups and analyzed their correlation with ages ,duration ,psoriasis area and severity index (PASI) .Results The contents of CXCL9 and IL‐22 in active cases and stable cases were obviously higher than those in con‐trols respectively by statistical analysis ,there was significant difference (P< 0 .05) .The contents of CXCL9 and IL‐22 in active ca‐ses were obvious higher than those in stable cases ,there was significant difference(P< 0 .05) .Conclusion CXCL9 and IL‐22 may be involved in the pathogenesis of vitiligo vulgaris .
