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首页> 美国卫生研究院文献>PLoS Pathogens >HIV and HCV Activate the Inflammasome in Monocytes and Macrophages via Endosomal Toll-Like Receptors without Induction of Type 1 Interferon
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HIV and HCV Activate the Inflammasome in Monocytes and Macrophages via Endosomal Toll-Like Receptors without Induction of Type 1 Interferon

机译:HIV和HCV通过内吞性类受体激活单核细胞和巨噬细胞中的炎性体而不诱导1型干扰素。

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Innate immune sensing of viral infection results in type I interferon (IFN) production and inflammasome activation. Type I IFNs, primarily IFN-α and IFN-β, are produced by all cell types upon virus infection and promote an antiviral state in surrounding cells by inducing the expression of IFN-stimulated genes. Type I IFN production is mediated by Toll-like receptor (TLR) 3 in HCV infected hepatocytes. Type I IFNs are also produced by plasmacytoid dendritic cells (pDC) after sensing of HIV and HCV through TLR7 in the absence of productive pDC infection. Inflammasomes are multi-protein cytosolic complexes that integrate several pathogen-triggered signaling cascades ultimately leading to caspase-1 activation and generation pro-inflammatory cytokines including interleukin (IL)-18 and IL-1β. Here, we demonstrate that HIV and HCV activate the inflammasome, but not Type I IFN production, in monocytes and macrophages in an infection-independent process that requires clathrin-mediated endocytosis and recognition of the virus by distinct endosomal TLRs. Knockdown of each endosomal TLR in primary monocytes by RNA interference reveals that inflammasome activation in these cells results from HIV sensing by TLR8 and HCV recognition by TLR7. Despite its critical role in type I IFN production by pDCs stimulated with HIV, TLR7 is not required for inflammasome activation by HIV. Similarly, HCV activation of the inflammasome in monocytes does not require TLR3 or its downstream signaling adaptor TICAM-1, while this pathway leads to type I IFN in infected hepatocytes. Monocytes and macrophages do not produce type I IFN upon TLR8 or TLR7 sensing of HIV or HCV, respectively. These findings reveal a novel infection-independent mechanism for chronic viral induction of key anti-viral programs and demonstrate distinct TLR utilization by different cell types for activation of the type I IFN vs. inflammasome pathways of inflammation.
机译:病毒感染的先天免疫感应导致I型干扰素(IFN)产生和炎症小体活化。感染病毒后,所有细胞类型都会产生I型IFN,主要是IFN-α和IFN-β,并通过诱导IFN刺激的基因表达来促进周围细胞的抗病毒状态。 I型IFN的产生是由HCV感染的肝细胞中的Toll样受体(TLR)3介导的。在没有生产性pDC感染的情况下,通过TLR7检测到HIV和HCV后,浆细胞样树突状细胞(pDC)也会产生I型干扰素。炎症小体是多蛋白胞质复合物,整合了几种病原体触发的信号级联,最终导致caspase-1激活并产生促炎性细胞因子,包括白介素(IL)-18和IL-1β。在这里,我们证明,HIV和HCV在独立于感染的过程中激活单核细胞和巨噬细胞中的炎性小体,但不激活I型IFN的产生,该过程需要网格蛋白介导的内吞作用,并需要通过独特的内体TLR识别病毒。 RNA干扰敲低原代单核细胞中的每个内体TLR,揭示这些细胞中的炎性体活化是由TLR8引起的HIV感测和TLR7引起的HCV识别引起的。尽管TLR7在由HIV刺激的pDC产生的I型IFN产生中起着关键作用,但对于HIV的炎性体激活并不需要TLR7。同样,单核细胞中炎性体的HCV激活不需要TLR3或其下游信号转导接头TICAM-1,而该途径可在感染的肝细胞中导致I型干扰素。在TLR8或TLR7分别检测到HIV或HCV时,单核细胞和巨噬细胞不会产生I型干扰素。这些发现揭示了一种新的独立于感染的机制,可用于慢性病毒诱导关键的抗病毒程序,并证明了不同细胞类型对TLR的利用,从而激活了I型IFN与炎症的炎症途径。

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