北京大学学报(医学版) ›› 2024, Vol. 56 ›› Issue (5): 756-762. doi: 10.19723/j.issn.1671-167X.2024.05.002
Jiang JIN*(), Xue CHEN, Yan ZHAO, Jun JIA, Jianzhong ZHANG
摘要:
目的: 探讨白细胞介素-25(interleukin-25,IL-25)对卵清蛋白(ovalbumin,OVA)诱导的特应性皮炎小鼠模型的影响,以及调控IL-25的意义。方法: 将90只健康雄性6周龄无特定病原体(specific pathogen free, SPF)级BALB/c小鼠分为6组(每组15只),分别为: ①皮下注射磷酸盐缓冲液(phosphate buffered saline, PBS)组(正常对照组); ②皮下注射小鼠IL-25组(IL-25组); ③皮下注射抗小鼠IL-25单克隆抗体组(anti-IL-25组),每日皮下注射1次×1周,间隔2周,重复每日皮下注射1次×1周,间隔2周,再重复每日皮下注射1次×1周,总共7周; ④ OVA致敏组(模型组); ⑤ OVA致敏及IL-25皮下注射组(IL-25干预致敏组); ⑥ OVA致敏及anti-IL-25注射组(anti-IL-25干预致敏组)。⑤⑥组在致敏过程中给予IL-25或anti-IL-25的方式同②③组。致敏期间观察比较小鼠的搔抓行为和皮肤表现,致敏结束24 h后由小鼠心脏取血,分离血清,采用酶联免疫吸附试验(enzyme linked immunosorbent assay, ELISA)检测总IgE、IL-4、IL-5、IL-13等。取致敏部位的皮肤进行苏木精-伊红(hematoxylin-eosin,HE)染色、免疫组织化学、实时PCR(real-time PCR)及Western blot检测。采用单因素(ANOVA)方差分析比较各组间各项指标的差异。结果: 实验小鼠末次处理24 h后,IL-25干预致敏组的搔抓次数高于模型组,anti-IL-25干预致敏组的搔抓行为显著低于模型组; IL-25干预致敏组特应性皮炎表现、表皮增厚及真皮炎细胞浸润程度均明显重于模型组及anti-IL-25干预致敏组; IL-25干预致敏组血清IgE、IL-4、IL-5、IL-13水平显著高于模型组及anti-IL-25干预致敏组; IL-25干预致敏组CD4+ T细胞在真皮层较anti-IL-25干预致敏组显著增多; IL-25干预致敏组的丝聚蛋白(filaggrin)及防御素β2(defensin β2)蛋白水平明显低于模型组或anti-IL-25干预致敏组。结论: 在OVA诱导的皮炎模型中,IL-25能够明显促进小鼠表皮屏障功能损害,加重OVA诱导的皮炎损害,拮抗IL-25可一定程度上缓解OVA诱导的皮炎损害。
中图分类号:
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