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首页> 外文期刊>Medical Microbiology and Immunology >American tegumentary leishmaniasis: T-cell differentiation profile of cutaneous and mucosal forms-co-infection with Trypanosoma cruzi
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American tegumentary leishmaniasis: T-cell differentiation profile of cutaneous and mucosal forms-co-infection with Trypanosoma cruzi

机译:美国皮肤性利什曼病:皮肤和粘膜形式的T细胞分化特征-克鲁氏锥虫共感染

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摘要

American tegumentary leishmaniasis displays two main clinical forms: cutaneous (CL) and mucosal (ML). ML is more resistant to treatment and displays a more severe and longer evolution. Since both forms are caused by the same Leishmania species, the immunological response of the host may be an important factor determining the evolution of the disease. Herein, we analyzed the differentiation and memory profile of peripheral CD4(+) and CD8(+) T lymphocytes of patients with CL and ML and their Leishmania-T. cruzi co-infected counterparts. We measured the expression of CD27, CD28, CD45RO, CD127, PD-1 and CD57, together with interferon-gamma and perforin. A highly differentiated phenotype was reflected on both T subsets in ML and preferentially on CD8(+) T cells in CL. A positive trend toward a higher T differentiation profile was found in T. cruzi-infected CL and ML patients as compared with Leishmania single infections. Association between CD8(+) T-cell differentiation and illness duration was found within the first year of infection, with progressive increase of highly differentiated markers over time. Follow-up of patients with good response to therapy showed predominance of early differentiated CD8(+) T cells and decrease of highly differentiated cells, while patients with frequent relapses presented the opposite pattern. CD8(+) T cells showed the most striking changes in their phenotype during leishmaniasis. Patients with long-term infections showed the highest differentiated degree implying a relation between T differentiation and parasite persistence. Distinct patterns of CD8(+) T differentiation during follow-up of different clinical outcomes suggest the usefulness of this analysis in the characterization of Leishmania-infected patients.
机译:美国皮状体利什曼病显示两种主要临床形式:皮肤(CL)和粘膜(ML)。 ML对治疗的抵抗力更强,并且表现出更严重,更长的进化。由于两种形式都是由相同的利什曼原虫物种引起的,因此宿主的免疫应答可能是决定疾病进展的重要因素。在这里,我们分析了CL和ML患者及其利什曼原虫-T患者外周血CD4(+)和CD8(+)T淋巴细胞的分化和记忆特性。克鲁兹共同感染的同行。我们测量了CD27,CD28,CD45RO,CD127,PD-1和CD57以及干扰素-γ和穿孔素的表达。高分化的表型反映在ML的两个T亚群上,并优先反映在CL的CD8(+)T细胞上。与利什曼原虫单一感染相比,克鲁斯氏锥虫感染的CL和ML患者发现了更高的T分化特征的积极趋势。在感染的第一年内发现了CD8(+)T细胞分化与疾病持续时间之间的关联,随着时间的推移,高分化标志物逐渐增加。对治疗反应良好的患者的随访显示,早期分化的CD8(+)T细胞占优势,高分化细胞减少,而频繁复发的患者则呈现相反的模式。 CD8(+)T细胞在利什曼病期间表现出最显着的变化。长期感染的患者表现出最高的分化程度,这暗示着T分化与寄生虫持久性之间的关系。在不同临床结果的随访过程中CD8(+)T分化的不同模式表明该分析在利什曼原虫感染患者的表征中的有用性。

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