HIV-1 induces NALP3-inflammasome expression and interleukin-1beta secretion in dendritic cells from healthy individuals but not from HIV-positive patients.

Pontillo A; Silva LT; Oshiro TM; Finazzo C; Crovella S; Duarte AJ

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HIV-1 induces NALP3-inflammasome expression and interleukin-1beta secretion in dendritic cells from healthy individuals but not from HIV-positive patients.

机译：HIV-1诱导健康个体而不是HIV阳性患者的树突状细胞中NALP3炎性体表达和白介素1β分泌。

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OBJECTIVE: NALP3-inflammasome is an innate mechanism, alternative to type-1 interferon, which is able to recognize nucleic acids and viruses in the cytoplasm and to induce pro-inflammatory response. Here, we hypothesized the involvement of inflammasome in the early defense against HIV-1 and in the full maturation of dendritic cells: for this, we evaluated the response of dendritic cells pulsed with HIV-1 in terms of inflammasome activation in healthy donors. Moreover, inflammasome response to HIV was evaluated in HIV-infected individuals. DESIGN AND METHODS: Monocyte-derived dendritic cells isolated from 20 healthy individuals (HC-DC) and 20 HIV-1-infected patients (HIV-DC) were pulsed with alditrithiol-2-inactivated HIV-1. We then analyzed inflammasome genes expression and interleukin-1beta (IL-1beta) secretion. RESULTS: In HC-DC, HIV-1 induced higher NLRP3/NALP3 mRNA expression compared with other inflammasome genes such as NALP1/NLRP1 or IPAF/NLRC4 (P < 0.001). This augmented expression was accompanied by CASP1-increased and IL1B-increased mRNA levels and by a significant increment of IL-1beta secretion (P < 0.05). Otherwise, HIV-1 failed to activate inflammasome and cytokine production in HIV-DC. HIV-DC showed an increased NLRP3/NALP3 basal expression, suggesting a chronic inflammatory profile of patients' immune cells. CONCLUSION: HIV-1 was able to induce a NALP3-inflammasome response in healthy individuals, indicating that this inflammasome could play a role in the first steps of HIV-1 infection; the consequent inflammatory process may be important for directing host immune response against the virus and/or disease progression. HIV-DC seemed to be chronically activated, but unresponsive against pathogens. Our findings could be of interest considering the ongoing research about dendritic cell manipulation and therapeutic strategies for AIDS involving dendritic cell-based immune-vaccines.

机译：目的：NALP3炎性小体是一种固有的机制，可替代1型干扰素，它能够识别细胞质中的核酸和病毒并诱导促炎反应。在这里，我们假设炎症小体参与了针对HIV-1的早期防御以及树突状细胞的完全成熟：为此，我们评估了健康捐献者中被HIV-1脉冲的树突状细胞在炎症小体活化方面的反应。此外，在感染了HIV的个体中评估了对HIV的炎症反应。设计与方法：对来自20名健康个体（HC-DC）和20名HIV-1感染患者（HIV-DC）的单核细胞衍生的树突状细胞进行Alditrithiol-2-灭活的HIV-1脉冲处理。然后，我们分析了炎症小体基因表达和白介素-1β（IL-1beta）分泌。结果：在HC-DC中，HIV-1诱导的NLRP3 / NALP3 mRNA表达高于其他炎性体基因，如NALP1 / NLRP1或IPAF / NLRC4（P <0.001）。这种增加的表达伴随着CASP1增加和IL1B增加的mRNA水平以及IL-1beta分泌的显着增加（P <0.05）。否则，HIV-1无法激活HIV-DC中的炎症小体和细胞因子的产生。 HIV-DC的NLRP3 / NALP3基础表达增加，提示患者免疫细胞呈慢性炎症。结论：HIV-1能够在健康个体中诱导NALP3炎性体反应，表明该炎性体可能在HIV-1感染的第一步中起作用。因此，炎症过程对于指导宿主针对病毒和/或疾病进展的免疫反应可能很重要。 HIV-DC似乎是慢性激活的，但对病原体没有反应。考虑到正在进行的有关树突细胞操作和涉及基于树突细胞的免疫疫苗的艾滋病治疗策略的研究，我们的发现可能是有意义的。

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《AIDS》 |2012年第1期|共8页
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Pontillo A; Silva LT; Oshiro TM; Finazzo C; Crovella S; Duarte AJ;
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1. HIV-1 induces NALP3-inflammasome expression and interleukin-1beta secretion in dendritic cells from healthy individuals but not from HIV-positive patients. [J] . Pontillo A, Silva LT, Oshiro TM, AIDS . 2012,第1期

机译：HIV-1诱导健康个体而不是HIV阳性患者的树突状细胞中NALP3炎性体表达和白介素1β分泌。
2. Cocaine Modulates Dendritic Cell-Specific C Type Intercellular Adhesion Molecule-3-Grabbing Nonintegrin Expression by Dendritic Cells in HIV-1 Patients. [J] . Nair MP, Mahajan SD, Schwartz SA, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2005,第11期

机译：可卡因通过HIV-1患者的树突状细胞调节树突状细胞特异性C型细胞间粘附分子3-捕获非整联蛋白的表达。
3. Leishmania infantum Amastigotes Enhance HIV-1 Production in Cocultures of Human Dendritic Cells and CD4+ T Cells by Inducing Secretion of IL-6 and TNF-α [J] . Ravendra Garg, Corinne Barat, Michel Ouellet, PLOS Neglected Tropical Diseases . 2009,第5期

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4. Reciprocal expressions of VEGF and the numbers of dendritic cells in arsenic-induced skin cancer: A plausible cause of impaired dendritic cell activation in arsenic carcinogenesis [C] . C.-H. Lee, C.-H. Hong, H.-S. Yu International Congress on Arsenic in the Environment . 2016

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5. The co-regulatory effect of extracellular matrix proteins and integrins with interleukin-1beta on cytokine secretion by epithelial cells. [D] . Lubin, Farah Dominique. 2001

机译：细胞外基质蛋白和整联蛋白与白介素-1β对上皮细胞分泌细胞因子的共调节作用。
6. Activated platelets induce secretion of interleukin-1beta monocyte chemotactic protein-1 and macrophage inflammatory protein-1alpha and surface expression of intercellular adhesion molecule-1 on cultured endothelial cells. [O] . J. K. Cha, M. H. Jeong, H. R. Bae, 2000

机译：活化的血小板诱导白介素-1β单核细胞趋化蛋白-1和巨噬细胞炎性蛋白-1α的分泌以及细胞间粘附分子-1在培养的内皮细胞上的表面表达。
7. HIV-1 induces NALP3-inflammasome expression and interleukin-1β secretion in dendritic cells from healthy individuals but not from HIV-positive patients. [O] . Pontillo A, Silva LT, Oshiro TM, 2012

机译：HIV-1诱导健康个体而不是HIV阳性患者的树突状细胞中NALP3炎性体表达和白介素1β分泌。

HIV-1 induces NALP3-inflammasome expression and interleukin-1beta secretion in dendritic cells from healthy individuals but not from HIV-positive patients.

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