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COX-2–PGE2 Signaling Impairs Intestinal Epithelial Regeneration and Associates with TNF Inhibitor Responsiveness in Ulcerative Colitis

机译：COX-2-PGE2信号传导危害肠上皮再生和患者抑制剂抑制剂患者患者溃疡性结肠炎的反应性

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Background: Inhibition of tumor necrosis factor-α (TNF) signaling is beneficial in the management of ulcerative colitis (UC), but up to one-third of patients do not have a clinical response of relevance to TNF inhibitors during induction therapy (i.e. primary non-responders [PNRs]). Through production of prostaglandins (PGs) and thromboxanes, cyclooxygenase-2 (COX-2) affects inflammation and epithelial regeneration and may in this way be implicated in treatment resistance to TNF inhibitors. Methods: In this study, COX-2 expression was analyzed in human intestinal biopsies and patient-derived monocytes, and the downstream consequences of COX-2 activity was evaluated by assessing the influence of the down-stream effector, PGE2, on intestinal epithelial stem cell self-renewal and differentiation using primary human intestinal organoids (“mini-guts”). Findings: We found that TNF stimulation induced COX-2 expression in monocytes isolated from responders (Rs), whereas COX-2 expression was constitutively high and non-inducible in monocytes from PNRs. Additionally, PGE2 in combination with proliferative signals transformed human intestinal epithelial cells to a proinflammatory state akin to flaring UC, whereas PGE2 in combination with differentiation signals supported robust mucin induction. Interpretation: Our work indicates that COX-2-PGE2 signaling could be a novel target for the management of PNRs to TNF inhibitors. We additionally demonstrate that COX-2–PGE2 signaling has dual functions during tissue repair and normal lineage differentiation, explaining in part the lack of response to TNF inhibitors among PNRs. Fund: This work was funded by grants from the Novo Nordisk Foundation, the Lundbeck Foundation, the Vanderbilt Digestive Disease Research Center, NIH Grants, Aase and Ejnar Danielsen's Foundation and the A.P. Møller Foundation. Keywords: COX-2, Intestinal epithelial cells, Monocytes, Prostaglandin E2, Ulcerative colitis

机译：背景：抑制肿瘤坏死因子-α（TNF）信号传导在溃疡性结肠炎（UC）的管理中是有益的，但最多三分之一的患者在感应治疗期间没有与TNF抑制剂相关的临床响应（即原发性非响应者[pnrs]）。通过生产前列腺素（PGS）和血栓素，环加氧基酶-2（COX-2）影响炎症和上皮再生，并且可以以这种方式涉及对TNF抑制剂的治疗抗性。方法：在该研究中，通过评估下流效应器PGE2，肠道上皮茎对肠上皮茎对肠道上皮茎的影响评估COX-2表达，在人肠活组织检查和患者衍生的单核细胞中分析了COX-2活性的下游后果使用初级人肠有机体（“迷你肠道”）的细胞自我更新和分化。结果：我们发现，TNF刺激诱导从响应者（RS）分离的单核细胞中的COX-2表达，而COX-2表达在来自PNR的单核细胞中构成高且不诱导。另外，PGE2与增殖性信号组合转化为类似于辐射UC的促炎状态转化为促炎状态，而PGE2与分化信号组合支持鲁棒粘蛋白诱导。解释：我们的作品表明COX-2-PGE2信令可以是对TNF抑制剂的PNR管理的新靶标。我们还证明Cox-2-PGE2信号传导在组织修复和正常谱系中具有双重功能，部分分化在PNR中对TNF抑制剂的反应缺乏响应。基金：这项工作由Novo Nordisk Foundation，Lundbeck Foundation，Vanderbift消化疾病研究中心，NIH赠款，Aase和EJNARDanielsen的基金会和A.P.Møller基金会的基金会提供资金。关键词：COX-2，肠上皮细胞，单核细胞，前列腺素E2，溃疡性结肠炎

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Yuan Li; Christoffer Soendergaard; Fredrik Holmberg Bergenheim; David M. Aronoff; Ginger Milne; Lene Buhl Riis; Jakob Benedict Seidelin; Kim B. Jensen; Ole Haagen Nielsen;
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1. COX-2–PGE2 Signaling Impairs Intestinal Epithelial Regeneration and Associates with TNF Inhibitor Responsiveness in Ulcerative Colitis [J] . Yuan Li, Christoffer Soendergaard, Fredrik Holmberg Bergenheim, EBioMedicine . 2018,第152期

机译：溃疡性结肠炎中COX-2–PGE2信号传导损害肠道上皮再生并与TNF抑制剂反应性相关
2. Adenine Inhibits TNF-alpha Signaling in Intestinal Epithelial Cells and Reduces Mucosal Inflammation in a Dextran Sodium Sulfate-Induced Colitis Mouse Model [J] . Fukuda Toshihiko, Majumder Kaustav, Zhang Hua, Journal of Agricultural and Food Chemistry . 2016,第21期

机译：腺嘌呤抑制肠上皮细胞中的TNF-α信号传导并减少葡聚糖硫酸钠诱导的结肠炎小鼠模型的粘膜炎症
3. gamma-Glutamyl cysteine and gamma-glutamyl valine inhibit TNF-alpha signaling in intestinal epithelial cells and reduce inflammation in a mouse model of colitis via allosteric activation of the calcium-sensing receptor [J] . Zhang Hua, Kovacs-Nolan Jennifer, Kodera Tomohiro, Biochimica et biophysica acta. Molecular basis of disease: BBA . 2015,第5期

机译：γ-谷氨酰胺半胱氨酸和γ-谷氨酰胺缬氨酸可抑制肠道上皮细胞中的TNF-α信号传导，并通过钙敏感受体的变构活化降低结肠炎小鼠模型的炎症
4. An Inflammation-responsive Hydrogel for Drug Delivery for Treatment of Ulcerative Colitis [C] . Sufeng Zhang, Joerg Ermann, Praveen Vemula, Society for Biomaterials annual meeting and exposition . 2013

机译：炎症反应水凝胶用于药物治疗溃疡性结肠炎
5. Regulation of COX-2 and PGE2-dependent recovery of intestinal barrier function [D] . Shifflett, Donnie Edward 2004

机译：调节COX-2和PGE2依赖性肠屏障功能的恢复
6. COX-2–PGE2 Signaling Impairs Intestinal Epithelial Regeneration and Associates with TNF Inhibitor Responsiveness in Ulcerative Colitis [O] . Yuan Li, Christoffer Soendergaard, Fredrik Holmberg Bergenheim, 2018

机译：溃疡性结肠炎中COX-2–PGE2信号传导损害肠道上皮再生并与TNF抑制剂反应相关。
7. Cholera Toxin B Subunit and Peptide LKEKK Inhibit TNF-α Signaling in Intestinal Epithelial Cells and Reduce Inflammation in a Mouse Model of Colitis [O] . 2019

机译：霍乱毒素B亚基和肽Lkekk抑制肠上皮细胞中TNF-α信号传导，降低结肠炎小鼠模型中的炎症

COX-2–PGE2 Signaling Impairs Intestinal Epithelial Regeneration and Associates with TNF Inhibitor Responsiveness in Ulcerative Colitis

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