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Treatment of experimental murine arthritis with transdermal photodynamic therapy

机译:用透皮光动力疗法治疗实验鼠关节炎

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Photodynamic therapy (PDT) using benzoporphyrin derivative, monoacid ring A (BPD), and transdermal light was able to significantly treat symptoms of adjuvant-enhanced arthritis in MRL-lpr mice. Clinical and histological evaluation showed that PDT was able to modify the progression of adjuvant-enhanced arthritis up to 10 days after induction. When PDT was used on arthritic joints displaying swelling, it prevented further deterioration of clinical symptoms (76%, 16/21). However, it did not significantly effect the histopathologic parameters. As we have previously reported that mitogen activated MRL-lpr splenocytes were shown to be more susceptible to in vitro PDT we postulate that our findings reflect a selective destruction of adjuvant activated lymphocytes in the circulation and/or joints. The application of PDT to eliminate activated cells responsible for the inflammatory reaction at the arthritic site may have significant clinical implications for the treatment of rheumatoid arthritis.
机译:光动力治疗(PDT)使用苯并卟啉衍生物,单酸环A(BPD)和透皮光,能够在MRL-LPR小鼠中显着地治疗佐剂增强关节炎的症状。临床和组织学评价显示PDT能够在诱导后10天改变佐剂增强关节炎的进展。当PDT用于表现出肿胀的关节炎关节时,它阻止了临床症状进一步恶化(76%,16/21)。但是,它没有显着影响组织病理学参数。由于我们之前报道了丝裂原激活的MRL-LPR脾细胞被证明更容易受到体外PDT的影响,我们假设我们的研究结果反映了循环和/或关节中的佐剂活性淋巴细胞的选择性破坏。 PDT在关节炎遗址上消除负责炎症反应的活性细胞的应用可能对类风湿性关节炎的治疗具有显着的临床意义。

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