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首页> 外文期刊>Journal of immunology research. >Evaluation of the Ability of Miltefosine Associated with Topical GM-CSF in Modulating the Immune Response of Patients with Cutaneous Leishmaniasis
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Evaluation of the Ability of Miltefosine Associated with Topical GM-CSF in Modulating the Immune Response of Patients with Cutaneous Leishmaniasis

机译:评价Miltefosine与局部GM-CSF相关的能力调节皮肤LeishManiaisis患者的免疫应答

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Cutaneous leishmaniasis (CL) due to L. braziliensis is associated with an exaggerated inflammatory response and tissue damage. Miltefosine is more effective than pentavalent antimony (Sbv) in the treatment of CL, and here, we evaluate the ability of Sbv, miltefosine, and GM-CSF administered intravenously, orally, or topically, respectively, to modify the immune response. Patients were treated with miltefosine plus GM-CSF, miltefosine plus placebo, or Sbv. Mononuclear cells were stimulated with soluble Leishmania antigen (SLA) on day 0 and day 15 of therapy, and cytokine levels were determined in supernatants by ELISA. The lymphocyte proliferation and oxidative burst were evaluated by flow cytometry, and the degree of infection and Leishmania killing by optical microscopy. Proliferation of CD4+ T cells were enhanced in patients using miltefosine and in CD8+ T cells when GM-CSF was associated. Enhancement in the oxidative burst occurred in the miltefosine plus GM-CSF group on day 15 of therapy. Moreover, the number of L. braziliensis in infected monocytes on day 15 as well as the percentage of infected cells was lower after 48- and 72-hour culture in cells from patients treated with miltefosine plus GM-CSF. In addition to the ability of miltefosine to kill Leishmania, the changes in the immune response caused by miltefosine and GM-CSF may increase the cure rate of CL patients using these drugs.
机译:由于L.Braziliensis引起的皮肤LeishManiaisis(CL)与夸张的炎症反应和组织损伤有关。 Miltefosine比PentAvalent锑(SBV)在治疗CL的静止(SBV)中更有效,在这里,我们评估SBV,MilteFOISINE和GM-CSF分别静脉内,口服或局部施用的能力以改变免疫应答。用Miltefosine加上GM-CSF,Miltefosine Plus安慰剂或SBV治疗患者。用溶解的Leishmania抗原(SLA)在治疗的第0天和第15天刺激单核细胞,并通过ELISA在上清液中测定细胞因子水平。通过流式细胞术评估淋巴细胞增殖和氧化突发,以及通过光学显微镜杀死的感染程度和杀菌程度。在使用Miltefosine和CD8 + T细胞的患者中,CD4 + T细胞的增殖增强了CD8 + T细胞,当GM-CSF相关时。在治疗第15天的Miltefosine Plus GM-CSF组中发生氧化突发的增强。此外,第15天感染的单核细胞中的L.Bariliensis的数量以及感染细胞的百分比后48-和72小时的细胞中的百分比较低,患有Miltefosine加上GM-CSF的患者的细胞中。除了Miltefosine杀死Leishmania的能力外,Miltefosine和GM-CSF引起的免疫应答的变化可能会增加CL患者使用这些药物的治愈率。

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