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LXR-dependent and -independent effects of oxysterols on immunity and tumor growth

机译:LXR-dependent和独立的影响oxysterols免疫和肿瘤生长

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摘要

Oxysterols are involved in maintaining cellular cholesterol levels. Recently, oxysterols have been demonstrated to modulate the function of immune cells and tumor growth. These effects can be dependent on the activation of the oxysterol-binding liver X receptors (LXRs) or, as recently demonstrated for T and B cells, DCs and neutrophils, can be independent of LXR activation. LXR-dependent oxysterol effects can be ascribed to the activation of LXRα, LXRβ or LXRαβ isoforms, which induces transcriptional activation or trans-repression of target genes. The prevalent activation of one isoform seems to be cell-, tissue-, or context-specific, as shown in some pathologic processes, i.e., infectious diseases, atherosclerosis, and autoimmunity. Oxysterol-LXR signaling has recently been shown to inhibit antitumor immune responses, as well as to modulate tumor cell growth. Here, we review the mechanisms that link oxysterols to tumor growth, and discuss possible networks at the basis of LXR-dependent and -independent oxysterol effects on immune cells and tumor development.
机译:Oxysterols参与维持细胞胆固醇水平。被证实能调节的功能免疫细胞和肿瘤生长。被依赖的激活oxysterol-binding肝X受体(LXRs)或,最近演示了T细胞和B细胞、DCs和中性粒细胞,可以独立于LXR激活。的激活归因于LXRα,LXRβLXRαβ亚型,导致转录目标基因的激活或trans-repression。一个同种型似乎普遍激活是细胞、组织或上下文相关,如图所示在某些病理过程,即具有传染性疾病、动脉粥样硬化和自身免疫。Oxysterol-LXR信号最近被证明抑制抗肿瘤免疫反应,以及调节肿瘤细胞的生长。链接oxysterols肿瘤的机制在增长,并讨论可能的网络LXR-dependent和独立oxysterol影响免疫细胞和肿瘤的发展。

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