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抗利什曼原虫药物调节原代人细胞中的 IL-12 表达和炎症小体激活。

Antileishmanial Drugs Modulate IL-12 Expression and Inflammasome Activation in Primary Human Cells.

机构信息

INSERM-U1124, Paris University, 75006 Paris, France.

Photeomix, 93160 Noisy Le Grand, France.

出版信息

J Immunol. 2020 Apr 1;204(7):1869-1880. doi: 10.4049/jimmunol.1900590. Epub 2020 Mar 4.

Abstract

Leishmaniases are neglected tropical diseases. The treatment of leishmaniasis relies exclusively on chemotherapy including amphotericin B (AmB), miltefosine (hexadecylphosphocholine), and pentamidine. Besides the fact that these molecules are harmful for patients, little is known about the impact of such antileishmanial drugs on primary human cells in relation to immune function. The present study demonstrates that all antileishmanial drugs inhibit CD4 and CD8 T cell proliferation at the doses that are not related to increased cell death. Our results highlight that antileishmanial drugs have an impact on monocytes by altering the expression of IL-12 induced by LPS, whereas only AmB induced IL-10 secretion; both cytokines are essential in regulating Th1 cell-mediated immunity. Interestingly, IL-12 and anti-IL-10 Abs improved T cell proliferation inhibited by AmB. Furthermore, our results show that in contrast to hexadecylphosphocholine and pentamidine, AmB induced gene expression of the inflammasome pathway. Thus, AmB induced IL-1β and IL-18 secretions, which are reduced by specific inhibitors of caspase activation (Q-VD) and NLRP3 activation (MCC950). Our results reveal previously underestimated effects of antileishmanial drugs on primary human cells.

摘要

利什曼病是被忽视的热带病。利什曼病的治疗完全依赖于化疗,包括两性霉素 B(AmB)、米替福新(十六烷基磷酸胆碱)和喷他脒。除了这些分子对患者有害之外,人们对这些抗利什曼病药物对与免疫功能相关的原发性人体细胞的影响知之甚少。本研究表明,所有抗利什曼病药物在与增加细胞死亡无关的剂量下抑制 CD4 和 CD8 T 细胞的增殖。我们的结果强调,抗利什曼病药物通过改变 LPS 诱导的 IL-12 的表达来影响单核细胞,而只有 AmB 诱导 IL-10 的分泌;这两种细胞因子在调节 Th1 细胞介导的免疫中都是必不可少的。有趣的是,IL-12 和抗 IL-10 Abs 改善了 AmB 抑制的 T 细胞增殖。此外,我们的结果表明,与十六烷基磷酸胆碱和喷他脒不同,AmB 诱导了炎症小体途径的基因表达。因此,AmB 诱导了 IL-1β 和 IL-18 的分泌,而 caspase 激活(Q-VD)和 NLRP3 激活(MCC950)的特异性抑制剂降低了它们的分泌。我们的结果揭示了抗利什曼病药物对原发性人体细胞的先前被低估的影响。

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