Kim Kyeong Hwan, Kim Dong Hyun, Jeong Hyun Jeong, Ryu Jin Suk, Kim Yu Jeong, Oh Joo Youn, Kim Mee Kum, Wee Won Ryang
Laboratory of Ocular Regenerative Medicine and Immunology, Seoul Artificial Eye Center, Seoul National University Hospital Biomedical Research Institute, Seoul, Korea.
Department of Ophthalmology, Haeundae Paik Hospital, Busan, Korea.
PLoS One. 2017 Aug 24;12(8):e0183678. doi: 10.1371/journal.pone.0183678. eCollection 2017.
Extracellular high mobility group box 1 (HMGB1) acts as a damage associated molecular pattern molecule through the Toll-like receptor to promote autoreactive B cell activation, which may be involved in the pathogenesis of Sjӧgren's syndrome. The aim of this study was to investigate the effect of subconjunctival administration of anti-HMGB1 on dry eye in a mouse model of Sjӧgren's syndrome.
Ten weeks-old NOD.B10.H2b mice were subconjunctivally injected with 0.02 to 2 μg of anti-HMGB1 antibodies or PBS twice a week for two consecutive weeks. Tear volume and corneal staining scores were measured and compared between before- and after-treatment. Goblet cell density was counted in PAS stained forniceal conjunctiva and inflammatory foci score (>50 cells/focus) was measured in extraorbital glands. Flow cytometry was performed to evaluate the changes in BrdU+ cells, IL-17-, IL-10-, or IFNγ-secreting cells, functional B cells, and IL-22 secreting innate lymphoid cells (ILC3s) in cervical lymph nodes. The level of IL-22 in intraorbital glands was measured by ELISA.
Injection of 2 μg or 0.02 μg anti-HMGB1 attenuated corneal epithelial erosions and increased tear secretion (p<0.05). Goblet cell density was increased in 0.2 μg and 2 μg anti-HMGB1-treated-mice with marginal significance. The inflammatory foci score, and the number of BrdU+ cells, IL-17-, IL-10-, IFNγ-secreting cells, and functional B cells did not significantly change following anti-HMGB1 treatment. Surprisingly, the percentage of ILC3s was significantly increased in the draining lymph nodes (p<0.05), and the expression of IL-22 was significantly increased in the intraorbital glands (p<0.05) after administration of 2 μg anti-HMGB1.
This study shows that subconjunctival administration of anti-HMGB1 attenuates clinical manifestations of dry eye. The improvement of dry eye may involve an increase of ILC3s, rather than modulation of B or plasma cells, as shown using a mouse model of Sjӧgren's syndrome.
细胞外高迁移率族蛋白B1(HMGB1)通过Toll样受体作为损伤相关分子模式分子,促进自身反应性B细胞活化,这可能参与干燥综合征的发病机制。本研究旨在探讨结膜下注射抗HMGB1对干燥综合征小鼠模型干眼的影响。
10周龄的NOD.B10.H2b小鼠每周两次结膜下注射0.02至2μg抗HMGB1抗体或PBS,连续两周。测量并比较治疗前后的泪液体积和角膜染色评分。对PAS染色的穹窿结膜进行杯状细胞密度计数,并对眶外腺的炎症灶评分(>50个细胞/灶)进行测量。采用流式细胞术评估颈部淋巴结中BrdU+细胞、分泌IL-17、IL-10或IFNγ的细胞、功能性B细胞以及分泌IL-22的固有淋巴细胞(ILC3s)的变化。通过ELISA检测眶内腺中IL-22的水平。
注射2μg或0.02μg抗HMGB1可减轻角膜上皮糜烂并增加泪液分泌(p<0.05)。0.2μg和2μg抗HMGB1治疗的小鼠杯状细胞密度增加,具有边缘显著性。抗HMGB1治疗后,炎症灶评分以及BrdU+细胞、分泌IL-17、IL-10、IFNγ的细胞和功能性B细胞的数量无显著变化。令人惊讶的是,注射2μg抗HMGB1后,引流淋巴结中ILC3s的百分比显著增加(p<0.05),眶内腺中IL-22的表达显著增加(p<0.05)。
本研究表明结膜下注射抗HMGB1可减轻干眼的临床表现。如在干燥综合征小鼠模型中所示,干眼的改善可能涉及ILC3s的增加,而非B细胞或浆细胞的调节。
Zotero 插件
