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IL-6-driven FasL promotes NF-κBp65/PUMA-mediated apoptosis in portal hypertensive gastropathy

机译：IL-6驱动的FasL促进门脉高压性胃病中NF-κBp65/ PUMA介导的细胞凋亡

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摘要

Mucosal epithelial apoptosis with non-specific inflammation is an essential pathological characteristic in portal hypertensive gastropathy (PHG). However, whether a coordinated crosstalk between myeloid cells and epithelial cells involved in PHG remains unclear. IL-6, which is induced in the mucosa of PHG patients and mice, promotes FasL production via enhancing NF-κBp65 activation in myeloid cells, while blockage of IL-6 signaling by Tocilizumab or deletion of NF-κBp65 in myeloid cells attenuates the inflammatory response and Fas/FasL-mediated epithelial apoptosis in PHG. IL-6-driven FasL from myeloid cells combines with epithelial Fas receptor to encourage NF-κBp65/PUMA-mediated epithelial apoptosis in PHG, and inhibition of NF-κBp65 or knockout of PUMA alleviates Fas/FasL-mediated epithelial apoptosis in PHG. These results indicate that IL-6 drives FasL generation via NF-κBp65 in myeloid cells to promote Fas/NF-κBp65/PUMA-mediated epithelial apoptosis in PHG, and this coordinated crosstalk between myeloid cells and epithelial cells may provide a potential therapeutic target for PHG.

机译：具有非特异性炎症的粘膜上皮细胞凋亡是门脉高压性胃病（PHG）的基本病理特征。但是，尚不清楚参与PHG的髓样细胞和上皮细胞之间是否存在协调的串扰。在PHG患者和小鼠的粘膜中诱导的IL-6通过增强髓样细胞中的NF-κBp65活化来促进FasL的产生，而通过Tocilizumab阻断IL-6信号传导或在髓样细胞中缺失NF-κBp65则减轻了炎症反应。 PHG中的应答和Fas / FasL介导的上皮细胞凋亡。来自髓样细胞的IL-6驱动的FasL与上皮Fas受体结合，促进NF-κBp65/ PUMA介导的PHG上皮细胞凋亡，而NF-κBp65的抑制或PUMA的敲除可减轻Fas / FasL介导的PHG上皮细胞凋亡。这些结果表明IL-6通过髓样细胞中的NF-κBp65驱动FasL生成，从而促进PHG中Fas /NF-κBp65/ PUMA介导的上皮细胞凋亡，而这种髓样细胞与上皮细胞之间的协同串扰可能为潜在的治疗靶点PHG。

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期刊名称 Cell Death Disease
作者
Siwei Tan; Minyi Xu; Bilun Ke; Yu Lu; Huiling Liu; Jie Jiang; Bin Wu;
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作者单位

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年(卷),期 2019(10),10
年度 2019
页码 748
总页数 18
原文格式 PDF
正文语种
中图分类细胞生物学;
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专利

1. IL-6-driven FasL promotes NF-κBp65/PUMA-mediated apoptosis in portal hypertensive gastropathy [J] . Siwei Tan, Minyi Xu, Bilun Ke, Cell death & disease. . 2019,第10期

机译：IL-6驱动的FasL促进门静脉高血压胃病中NF-κBP65/ PUMA介导的凋亡
2. beta-Arrestin-1 protects against endoplasmic reticulum stress/p53-upregulated modulator of apoptosis-mediated apoptosis via repressing p-p65/inducible nitric oxide synthase in portal hypertensive gastropathy [J] . Tan Siwei, Li Leijia, Chen Tingting, Free Radical Biology and Medicine: The Official Journal of the Oxygen Society . 2015,第Null期

机译：β-Arrestin-1通过抑制p-p65 /诱导型一氧化氮合酶预防内质网应激/ p53上调的细胞凋亡介导的凋亡调节剂
3. Aminoguanidine corrects hyperdynamic circulation without ameliorating portal hypertension and portal hypertensive gastropathy in anesthetized portal hypertensive rats. [J] . Lee FY, Wang SS, Tsai YT, Journal of Hepatology: The Journal of the European Association for the Study of the Liver . 1997,第3期

机译：氨基胍可改善麻醉性门脉高压大鼠的门脉高压，而不会改善门脉高压和门脉高压性胃病。
4. Fas/FasL mediates NF-κBp65/PUMA-modulated hepatocytes apoptosis via autophagy to drive liver fibrosis [O] . Siwei Tan, Xianzhi Liu, Lingjun Chen, 2021

机译：Fas / FasL通过自噬介导NF-κBP65/ PUMA调节的肝细胞细胞凋亡以驱动肝纤维化
5. IL-6-driven FasL promotes NF-κBp65/PUMA-mediated apoptosis in portal hypertensive gastropathy [O] . Siwei Tan, Minyi Xu, Bilun Ke, 2019

机译：IL-6驱动的FasL促进门静脉高血压胃病中NF-κBP65/ PUMA介导的凋亡

IL-6-driven FasL promotes NF-κBp65/PUMA-mediated apoptosis in portal hypertensive gastropathy

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