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控制(天然)和氧化(DeMP)线粒体 RNA 是人类中的促炎调节因子。

Control (Native) and oxidized (DeMP) mitochondrial RNA are proinflammatory regulators in human.

机构信息

Wadsworth Center, New York State Department of Health, Albany, NY, 12201, USA.

Department of Immunology and Microbial Disease, Albany Medical College, Albany, NY, 12208, USA.

出版信息

Free Radic Biol Med. 2019 Nov 1;143:62-69. doi: 10.1016/j.freeradbiomed.2019.07.019. Epub 2019 Jul 19.

Abstract

Inflammation is implicated in a wide range of disorders, and thought to be involved in most leading causes of death today in the United States with high associated costs. New insights into better understanding its etiology, detection and prevention are thus of major importance in health care. One emerging field providing such insights has been the identification of DAMPs, or damage-associated molecular patterns. We have studied DAMPs within the context of degraded and oxidized mitochondrial DNA and RNA ("DeMP"), most recently demonstrating potent mitochondrial RNA (mtRNA) immunogenic response in mouse macrophages. Here, we extend these studies to assess the proinflammatory role of mitochondrial control (native) and oxidized RNA using human RNA and cells. THP-1 macrophage mtRNA triggered a proinflammatory response (induction of IL-6 and TNFα) when transfected into the same cells. Modestly oxidized mtRNA (DeMP RNA) but not cytoplasmic RNA induced a similar response, in contrast to attenuated immunogenicity previously observed with more oxidized DeMP RNA. This DeMP RNA may also cause a mild prooxidant stress. The proinflammatory effects of mtRNA was significantly reduced following pretreatment with RNases specific for single and double stranded RNA, implicating these forms of mtRNA in proinflammatory response. The natural nucleic acid-encapsulating peptide LL-37 also triggered a proinflammatory effect in the presence of control mtRNA and DeMP RNA. Finally, human blood plasma RNA exhibits proinflammatory activity. These results provide new insights into the immunostimulation of mitochondrial RNA including its activity in human cells; identify human plasma RNA as proinflammatory; and provide further evidence that oxidized DeMP mtRNA acts as a sensitive and broad-spectrum sensor and regulator of mitochondrial oxidative stress.

摘要

炎症与广泛的疾病有关,被认为与当今美国大多数主要死亡原因有关,而且成本高昂。因此,更好地了解其病因、检测和预防方法的新见解对医疗保健至关重要。一个提供此类见解的新兴领域是 DAMPs(损伤相关分子模式)的识别。我们已经在降解和氧化的线粒体 DNA 和 RNA(“DeMP”)的背景下研究了 DAMPs,最近在小鼠巨噬细胞中证明了强大的线粒体 RNA(mtRNA)免疫原性反应。在这里,我们扩展了这些研究,以评估使用人 RNA 和细胞的线粒体控制(天然)和氧化 RNA 的促炎作用。当转染到相同的细胞中时,THP-1 巨噬细胞 mtRNA 引发了促炎反应(IL-6 和 TNFα 的诱导)。适度氧化的 mtRNA(DeMP RNA)而不是细胞质 RNA 诱导了类似的反应,与以前观察到的更氧化的 DeMP RNA 的免疫原性减弱形成对比。这种 DeMP RNA 也可能引起轻微的促氧化剂应激。在用针对单链和双链 RNA 的 RNase 预处理后,mtRNA 的促炎作用显著降低,这表明这些形式的 mtRNA 参与了促炎反应。天然核酸包裹肽 LL-37 也在存在对照 mtRNA 和 DeMP RNA 的情况下引发了促炎作用。最后,人血浆 RNA 表现出促炎活性。这些结果为线粒体 RNA 的免疫刺激提供了新的见解,包括其在人细胞中的活性;确定人血浆 RNA 具有促炎作用;并提供进一步的证据表明氧化的 DeMP mtRNA 作为线粒体氧化应激的敏感和广谱传感器和调节剂起作用。

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