首页> 外文会议>Optical Methods for Tumor Treatment and Detections: Mechanisms and Techniques in Photodynamic Therapy VII >Interleukin-12 reverses the inhibitory impact of photodynamic therapy (PDT) on the murine contact hypersensitivity response
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Interleukin-12 reverses the inhibitory impact of photodynamic therapy (PDT) on the murine contact hypersensitivity response

机译:白介素12逆转光动力疗法(PDT)对小鼠接触超敏反应的抑制作用

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Abstract: Treatment of mice with certain photosensitizers combined with exposure to visible light limits the development of the immunologically-mediated contact hypersensitivity (CHS) response against topically-applied chemical haptens. Understanding of the inhibitory action of photosensitizers upon the CHS response is incomplete. Benzoporphyrin derivative monoacid ring A (BPD-MA, verteporfin), a photosensitizer with immunomodulatory activity, strongly depressed CHS responses to the hapten dinitrofluorobenzene (DNFB). However, if mice were administered 1 $mu@g of a recombinant preparation of the pro- inflammatory cytokine interleukin-12 (rIL-12), full-fledged CHS responses to DNFB ensued in animals treated with BPD-MA and light. In contrast, when rIL-12 was given in combination with an anti-IL-12 antibody the restorative effect of rIL-12 on the CHS response of PDT-treated mice was blocked. Evaluation of the cytokine status of spleen and draining lymph node cells showed for DNFB painted animals, that the release of the immunosuppressive cytokine IL-10 was increased by PDT and rIL-12 counter-acted the increase in IL-10 liberation associated with PDT. These studies indicate that IL-10 formation is upregulated and the availability of IL-12 may be limited in mice treated with PDT. These features may contribute to deficient CHS responses observed with PDT. !41
机译:摘要:用某些光敏剂与暴露于可见光的组合治疗小鼠,限制了针对局部应用的化学半抗原的免疫介导的接触超敏反应(CHS)反应的发展。对光敏剂对CHS反应的抑制作用的了解还不完全。具有免疫调节活性的光敏剂苯并卟啉衍生物单酸环A(BPD-MA,verteporfin)强烈抑制了CHS对半抗原二硝基氟苯(DNFB)的反应。但是,如果给小鼠注射1μg促炎细胞因子白细胞介素12(rIL-12)的重组制剂,则在用BPD-MA和光照治疗的动物中,CHS对DNFB的反应就会成熟。相反,当将rIL-12与抗IL-12抗体联合使用时,rIL-12对PDT处理的小鼠的CHS反应的修复作用被阻断。 DNFB涂染动物的脾脏和引流淋巴结细胞的细胞因子状态评估表明,PDT可增加免疫抑制性细胞因子IL-10的释放,而rIL-12可抵消与PDT相关的IL-10释放的增加。这些研究表明,在用PDT治疗的小鼠中,IL-10的表达上调并且IL-12的可用性可能受到限制。这些功能可能会导致PDT观察到的CHS反应不足。 !41

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