<p>Oral lichen planus (OLP) is a prevalent T-cell-mediated inflammatory disease of the human oral mucosa. Intraepithelial lymphocytes (IELs) engage in close cellular interactions with epithelial keratinocytes; however, the molecular mechanisms governing their migration and dynamic crosstalk with the epithelium remain incompletely defined. Here, we demonstrate that TCRαβ<sup>+</sup>CD8αα<sup>+</sup> and TCRγδ<sup>+</sup>CD8αα<sup>+</sup> IELs represent two key CD8αα<sup>+</sup> subsets within the total IEL population in OLP lesions. Live-cell imaging revealed that CD8αα⁻ IELs exhibited slower migratory kinetics compared with their CD8αα<sup>+</sup> counterparts, confirming that surface CD8αα expression facilitates epithelial migration of CD8<sup>+</sup> IELs. Within inflamed OLP mucosa, CD8αα<sup>+</sup> IELs produce markedly elevated levels of the pro-inflammatory cytokines IL-17&#xa0;A and IFN-γ. Neutralization of these two cytokines with specific antibodies reduced the migratory capacity of both CD8αα<sup>+</sup> and CD8αα⁻ IELs, indicating that the inflammatory microenvironment promoted CD8<sup>+</sup> IEL recruitment into lesional epithelium. GPR55 was highly expressed in CD8αα<sup>+</sup> IELs. Pharmacological blockade of GPR55 suppressed proliferation and significantly induced apoptosis in both IEL subsets. Furthermore, GPR55 antagonism robustly enhanced IEL migration and strengthened cell-to-cell contacts between IELs and oral keratinocytes (KCs). These findings identify GPR55 as a negative regulator that restricts transmigration of CD8<sup>+</sup> IELs into the oral epithelium. Targeted GPR55 inhibition may represent a promising strategy to modulate aberrant IEL activity and preserve mucosal epithelial barrier integrity in OLP.</p>

错误:搜索内容不能为空,请输入英文关键词
错误:关键词超出字数限制,请精简
高级检索

GPR55 negatively regulates CD8+ intraepithelial lymphocyte migration dynamics in oral lichen planus

  • Dongyang Zhou,
  • Gang Zhou

摘要

Oral lichen planus (OLP) is a prevalent T-cell-mediated inflammatory disease of the human oral mucosa. Intraepithelial lymphocytes (IELs) engage in close cellular interactions with epithelial keratinocytes; however, the molecular mechanisms governing their migration and dynamic crosstalk with the epithelium remain incompletely defined. Here, we demonstrate that TCRαβ+CD8αα+ and TCRγδ+CD8αα+ IELs represent two key CD8αα+ subsets within the total IEL population in OLP lesions. Live-cell imaging revealed that CD8αα⁻ IELs exhibited slower migratory kinetics compared with their CD8αα+ counterparts, confirming that surface CD8αα expression facilitates epithelial migration of CD8+ IELs. Within inflamed OLP mucosa, CD8αα+ IELs produce markedly elevated levels of the pro-inflammatory cytokines IL-17 A and IFN-γ. Neutralization of these two cytokines with specific antibodies reduced the migratory capacity of both CD8αα+ and CD8αα⁻ IELs, indicating that the inflammatory microenvironment promoted CD8+ IEL recruitment into lesional epithelium. GPR55 was highly expressed in CD8αα+ IELs. Pharmacological blockade of GPR55 suppressed proliferation and significantly induced apoptosis in both IEL subsets. Furthermore, GPR55 antagonism robustly enhanced IEL migration and strengthened cell-to-cell contacts between IELs and oral keratinocytes (KCs). These findings identify GPR55 as a negative regulator that restricts transmigration of CD8+ IELs into the oral epithelium. Targeted GPR55 inhibition may represent a promising strategy to modulate aberrant IEL activity and preserve mucosal epithelial barrier integrity in OLP.