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Hypoxia attenuates purinergic P2X receptor-induced inflammatory gene expression in brainstem microglia

机译：缺氧减弱嘌呤能P2X受体诱导的脑干小胶质细胞的炎症基因表达

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Hypoxia and increased extracellular nucleotides are frequently coincident in the brainstem. Extracellular nucleotides are potent modulators of microglial inflammatory gene expression via P2X purinergic receptor activation. Although hypoxia is also known to modulate inflammatory gene expression, little is known about how hypoxia or P2X receptor activation alone affects inflammatory molecule production in brainstem microglia, nor how hypoxia and P2X receptor signaling interact when they occur together. In the study reported here, we investigated the ability of a brief episode of hypoxia (2 hours) in the presence and absence of the nonselective P2X receptor agonist 2′(3′)-O-(4-benzoylbenzoyl)adenosine-5′-triphosphate (BzATP) to promote inflammatory gene expression in brainstem microglia in adult rats. We evaluated inducible nitric oxide synthase (iNOS), tumor necrosis factor alpha (TNFα), and interleukin (IL)-6 messenger RNA levels in immunomagnetically isolated brainstem microglia. While iNOS and IL-6 gene expression increased with hypoxia and BzATP alone, TNFα expression was unaffected. Surprisingly, BzATP-induced inflammatory effects were lost after hypoxia, suggesting that hypoxia impairs proinflammatory P2X-receptor signaling. We also evaluated the expression of key P2X receptors activated by BzATP, namely P2X1, P2X4, and P2X7. While hypoxia did not alter their expression, BzATP upregulated P2X4 and P2X7 mRNAs; these effects were ablated in hypoxia. Although both P2X4 and P2X7 receptor expression correlated with increased microglial iNOS and IL-6 levels in microglia from normoxic rats, in hypoxia, P2X7 only correlated with IL-6, and P2X4 correlated only with iNOS. In addition, correlations between P2X7 and P2X4 were lost following hypoxia, suggesting that P2X4 and P2X7 receptor signaling differs in normoxia and hypoxia. Together, these data suggest that hypoxia suppresses P2X receptor-induced inflammatory gene expression, indicating a potentially immunosuppressive role of extracellular nucleotides in brainstem microglia following exposure to hypoxia.

机译：缺氧和细胞外核苷酸增加经常在脑干中同时发生。细胞外核苷酸是经由P2X嘌呤能受体激活的小神经胶质炎性基因表达的有效调节剂。尽管还已知缺氧会调节炎症基因的表达，但对缺氧或P2X受体的活化如何单独影响脑干小胶质细胞中炎症分子产生的了解，以及缺氧和P2X受体的信号传导同时发生时如何相互作用的知之甚少。在此处报告的研究中，我们研究了在存在和不存在非选择性P2X受体激动剂2'（3'）-O-（4-苯甲酰基苯甲酰基）腺苷-5'-的情况下短暂缺氧（2小时）的能力三磷酸（BzATP）促进成年大鼠脑干小胶质细胞中炎症基因的表达。我们评估了免疫磁分离的脑干小胶质细胞中的诱导型一氧化氮合酶（iNOS），肿瘤坏死因子α（TNFα）和白介素（IL）-6信使RNA水平。尽管仅缺氧和BzATP会增加iNOS和IL-6基因的表达，但TNFα的表达不会受到影响。令人惊讶的是，缺氧后BzATP诱导的炎症作用消失了，这表明缺氧损害了促炎性P2X受体信号传导。我们还评估了由BzATP激活的关键P2X受体的表达，即P2X1，P2X4和P2X7。低氧不会改变其表达，但BzATP上调了P2X4和P2X7 mRNA。这些作用在缺氧时被消除。尽管P2X4和P2X7受体的表达均与常氧大鼠小胶质细胞中的小胶质iNOS和 IL-6 水平相关，但在缺氧时， P2X7 仅与 IL-6相关和 P2X4 仅与 iNOS 相关。另外，缺氧后 P2X7 和 P2X4 之间的相关性消失，这表明 P2X4 和 P2X7 受体信号在常氧和低氧。总之，这些数据表明缺氧抑制P2X受体诱导的炎症基因表达，表明缺氧后脑干小胶质细胞外核苷酸可能具有免疫抑制作用。 展开▼

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期刊名称 Hypoxia

作者
Stephanie MC Smith; Gordon S Mitchell; Scott A Friedle; Christine M Sibigtroth; Stéphane Vinit; Jyoti J Watters;
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年(卷),期 2013(1),-1

年度 2013

页码 1–11

总页数 11

原文格式 PDF

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关键词
P2X4 P2X7 P2X1 BzATP inflammation cytokine;

机译：P2X4;P2X7;P2X1;BzATP;炎症;细胞因子;

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专利

1. Hypoxia attenuates purinergic P2X receptor-induced inflammatory gene expression in brainstem microglia [J] . Stephanie MC Smith, Gordon S Mitchell, Scott A Friedle, Hypoxia . 2013,第4期

机译：缺氧减弱嘌呤能P2X受体诱导的脑干小胶质细胞的炎症基因表达

2. Sulforaphane induces Nrf2 target genes and attenuates inflammatory gene expression in microglia from brain of young adult and aged mice [J] . Townsend Brigitte E., Johnson Rodney W. Experimental Gerontology . 2016,第Null期

机译：萝卜硫烷诱导成年小鼠和成年小鼠脑中小胶质细胞中Nrf2靶基因并减弱炎症基因表达

3. Pro-inflammatory gene expression and neurotoxic effects of activated microglia are attenuated by absence of CCAAT/enhancer binding protein β [J] . Marco Straccia, Núria Gresa-Arribas, Guido Dentesano, Journal of neuroinflammation . 2011,第1期

机译：CCAAT /增强子结合蛋白β的缺失减弱了活化的小胶质细胞的促炎基因表达和神经毒性作用

4. The treatment with non-thermal plasma on human keratinocyte can block TNF-α and IFN-γ mediated pro-inflammatory gene expressions [C] . Choi Jeong-Hae, Lee Hae-June, Hong Jin-Woo, IEEE International Conference on Plasma Sciences . 2015

机译：非热血浆对人角质形成细胞的治疗可阻断TNF-α和IFN-γ介导的促炎基因表达

5. Mechanisms of Purinergic Receptor 2X Modulation of Microglial Gene Expression: Influence of Hypoxia and Re-Oxygenation. [D] . Friedle, Scott Alan. 2010

机译：嘌呤能受体2X调节小胶质细胞基因表达的机制：缺氧和再充氧的影响。

6. Sulforaphane induces Nrf2 target genes and attenuates inflammatory gene expression in microglia from brain of young adult and aged mice [O] . Brigitte E. Townsend, Rodney W. Johnson -1

机译：萝卜硫素诱导成年小鼠和成年小鼠脑中小胶质细胞中的Nrf2靶基因并减弱炎症基因的表达

7. Sulforaphane induces Nrf2 target genes and attenuates inflammatory gene expression in microglia from brain of young adult and aged mice [O] . Brigitte E. Townsend, Rodney W. Johnson 2016

机译：亚氟烃诱导NRF2靶基因，并从年轻成人和老年小鼠的脑中衰减小胶质细胞中的炎症基因表达

1. NaHS对ATP诱导大鼠小胶质细胞P2X受体表达的影响 [J] . 马洁 ,郭康 ,吕林亚 . 中国应用生理学杂志 . 2017,第006期

2. MicroRNA-182靶向抑制TLR4后减轻缺氧诱导的小胶质细胞炎症反应 [J] . 汪继 ,赵浩 ,陈秀芬 . 中华神经创伤外科电子杂志 . 2019,第003期

3. MicroRNA-182靶向抑制TLR4后减轻缺氧诱导的小胶质细胞炎症反应 [J] . 汪继1 ,赵浩1 ,陈秀芬1 . 中华神经创伤外科电子杂志 . 2019,第003期

4. 清开灵对小胶质细胞缺氧活化诱导的脑微血管内皮细胞Toll样受体4、gp91phox和闭锁小带蛋白-1表达的影响 [J] . 田超 ,玛娜璐璐 ,袁梦晨 . 中国康复理论与实践 . 2019,第011期

5. 载脂蛋白E和Ⅱ型髓系细胞受体在脂多糖诱导的小胶质细胞炎症反应中的作用 [J] . 陈翔 ,李广站 ,王玉琴 . 临床神经病学杂志 . 2021,第001期

6. 缺氧诱导大鼠肺泡上皮细胞凋亡与缺氧诱导因子-1 α相关基因表达的关系 [C] . 吕回 ,贺娟 . 中华医学会第二届全国重症医学大会 . 2007

7. 嘌呤受体P2X对大鼠缺氧缺糖损伤海马脑片/突触体谷氨酸与γ-氨基丁酸释放的调控作用 [A] . 景宇淼 . 2010

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2. P2X嘌呤能受体激动剂在增强胰腺β细胞中胰岛素分泌中的应用 [P] . 中国专利： CN102946887B . 2016.06.29

3. Process for suppressing expression of vcam-1 Process for suppressing expression of redox-sensitive gene Process for activating gene progress prediction or evaluation of diseases mediated by vcma-1 in vivo Process for predicting evaluation of disease mediated by sensitive gene around in vivo process for evaluation of vascular endothelial cell sensitivity process for selecting compounds process for treating cardiovascular disease process for suppressing expression of vcam-1 in human cells process for treating inflammatory skin disease process for treating human endothelial disease process for treating condition inflammatory and pharmaceutical composition [P] . 外国专利： BR9507716A . 1997-09-23

机译：抑制vcam-1表达的方法抑制氧化还原敏感基因表达的方法体内激活vcma-1介导的疾病的基因进展预测或评估的过程在体内评估过程中，预测由敏感基因介导的疾病的评估过程化合物的血管内皮细胞敏感性过程的选择治疗心血管疾病的过程抑制人细胞中vcam-1的表达的过程治疗炎症性皮肤病的过程治疗人类内皮病的过程治疗状况的炎症和药物组合物的过程

4. SCREENING METHOD USING, AS INDEX, EXPRESSION LEVEL OF LOX GENE IN HYPOXIA CONDITION, INCREASE INHIBITOR OF EXPRESSION OF LOX GENE, FIBROSIS INHIBITOR OF SUBCUTANEOUS FAT CELL, AND IMPROVEMENT OR PREVENTIVE AGENT OF SAGGING [P] . 外国专利： JP2019207232A . 2019-12-05

机译：以低氧状态下LOX基因的表达水平为指标的筛选方法，增加LOX基因表达的抑制因子，皮下脂肪细胞的纤维化抑制剂和下垂的改善或预防剂

5. A MICROORGANISM HAVING AN ATTENUATING MUTATION WHICH DISRUPTS THE EXPRESSION OF THE ssaV GENE AND AN ATTENUATING MUTATION WHICH DISRUPTS THE EXPRESSION OF THE aroC GENE [P] . 外国专利： IL146255B . 2008-11-26

机译：具有削弱ssaV基因表达的突变的微生物和具有衰减aroC基因表达的突变的微生物

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Hypoxia attenuates purinergic P2X receptor-induced inflammatory gene expression in brainstem microglia

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