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相似文献

1
Neutrophil-mediated changes in vascular permeability are inhibited by topical application of aspirin-triggered 15-epi-lipoxin A4 and novel lipoxin B4 stable analogues.局部应用阿司匹林触发的15-表-脂氧素A4和新型脂氧素B4稳定类似物可抑制中性粒细胞介导的血管通透性变化。
J Clin Invest. 1998 Feb 15;101(4):819-26. doi: 10.1172/JCI1578.
2
Aspirin-triggered 15-epi-lipoxin A4 (LXA4) and LXA4 stable analogues are potent inhibitors of acute inflammation: evidence for anti-inflammatory receptors.阿司匹林触发的15-表-脂氧素A4(LXA4)和LXA4稳定类似物是急性炎症的有效抑制剂:抗炎受体的证据。
J Exp Med. 1997 May 5;185(9):1693-704. doi: 10.1084/jem.185.9.1693.
3
Leukotriene B4 receptor transgenic mice reveal novel protective roles for lipoxins and aspirin-triggered lipoxins in reperfusion.白三烯B4受体转基因小鼠揭示了脂氧素和阿司匹林触发的脂氧素在再灌注中的新保护作用。
J Clin Invest. 1999 Aug;104(3):309-16. doi: 10.1172/JCI7016.
4
Lipoxin (LX)A4 and aspirin-triggered 15-epi-LXA4 inhibit tumor necrosis factor 1alpha-initiated neutrophil responses and trafficking: regulators of a cytokine-chemokine axis.脂氧素(LX)A4和阿司匹林触发的15-表-LXA4抑制肿瘤坏死因子1α引发的中性粒细胞反应和迁移:一种细胞因子-趋化因子轴的调节因子。
J Exp Med. 1999 Jun 21;189(12):1923-30. doi: 10.1084/jem.189.12.1923.
5
Lipoxin A4 and B4 inhibit leukotriene-stimulated interactions of human neutrophils and endothelial cells.脂氧素A4和B4可抑制白三烯刺激的人中性粒细胞与内皮细胞的相互作用。
J Immunol. 1996 Mar 15;156(6):2264-72.
6
Lipoxin A4 and aspirin-triggered 15-epi-lipoxin A4 inhibit human neutrophil migration: comparisons between synthetic 15 epimers in chemotaxis and transmigration with microvessel endothelial cells and epithelial cells.脂氧素A4和阿司匹林触发的15-表-脂氧素A4抑制人中性粒细胞迁移:合成的15个差向异构体在趋化性以及与微血管内皮细胞和上皮细胞跨膜迁移方面的比较
J Immunol. 2003 Mar 1;170(5):2688-94. doi: 10.4049/jimmunol.170.5.2688.
7
Selectivity of recombinant human leukotriene D(4), leukotriene B(4), and lipoxin A(4) receptors with aspirin-triggered 15-epi-LXA(4) and regulation of vascular and inflammatory responses.重组人白三烯D4、白三烯B4和脂氧素A4受体对阿司匹林触发的15-表-脂氧素A4的选择性以及血管和炎症反应的调节
Am J Pathol. 2001 Jan;158(1):3-9. doi: 10.1016/S0002-9440(10)63937-5.
8
Characterization of human neutrophil and endothelial cell ligand-operated extracellular acidification rate by microphysiometry: impact of reoxygenation.通过微生理测定法对人中性粒细胞和内皮细胞配体激活的细胞外酸化率进行表征:复氧的影响。
J Pharmacol Exp Ther. 1998 Apr;285(1):252-61.
9
Lipoxin A4 and lipoxin B4 stimulate the release but not the oxygenation of arachidonic acid in human neutrophils: dissociation between lipid remodeling and adhesion.脂氧素A4和脂氧素B4刺激人中性粒细胞中花生四烯酸的释放,但不影响其氧化:脂质重塑与黏附之间的分离。
J Cell Physiol. 1990 Jun;143(3):512-23. doi: 10.1002/jcp.1041430316.
10
Lipoxin A4 and aspirin-triggered 15-epi-LXA4 inhibit tumor necrosis factor-alpha-initiated neutrophil responses and trafficking: novel regulators of a cytokine-chemokine axis relevant to periodontal diseases.脂氧素A4和阿司匹林触发的15-表-脂氧素A4抑制肿瘤坏死因子-α引发的中性粒细胞反应和迁移:与牙周疾病相关的细胞因子-趋化因子轴的新型调节因子。
J Periodontal Res. 1999 Oct;34(7):370-3. doi: 10.1111/j.1600-0765.1999.tb02268.x.

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1
Aspirin in hepatocellular carcinoma: Is it an out-of-date or promising treatment?阿司匹林在肝细胞癌中的应用:它是一种过时的治疗方法还是有前景的治疗方法?
ILIVER. 2022 Mar 28;1(1):55-64. doi: 10.1016/j.iliver.2022.03.003. eCollection 2022 Mar.
2
Reprogramming inflammation: Mechanisms and therapeutic targeting of eicosanoids and pro-resolving mediators.炎症重编程:类花生酸和促消退介质的机制及治疗靶点
Eur J Pharmacol. 2025 Jul 5;1003:177924. doi: 10.1016/j.ejphar.2025.177924.
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The Importance of Resolvin D1, LXA4, and LTB4 in Patients with Acute Pancreatitis Due to Gallstones.消退素D1、脂氧素A4和白三烯B4在胆结石性急性胰腺炎患者中的重要性。
Medicina (Kaunas). 2025 Jan 29;61(2):239. doi: 10.3390/medicina61020239.
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A potent proresolving mediator 17R-resolvin D2 from human macrophages, monocytes, and saliva.人巨噬细胞、单核细胞和唾液中的一种强效促解决介质 17R- resolvin D2。
Sci Adv. 2024 Nov 22;10(47):eadq4785. doi: 10.1126/sciadv.adq4785. Epub 2024 Nov 20.
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Coronary microvascular dysfunction as a chronic inflammatory state: Is there a role for omega-3 fatty acid treatment?作为一种慢性炎症状态的冠状动脉微血管功能障碍:ω-3脂肪酸治疗是否起作用?
Am Heart J Plus. 2022 Jan 30;13:100098. doi: 10.1016/j.ahjo.2022.100098. eCollection 2022 Jan.
6
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A Stereocontrolled Total Synthesis of Lipoxin B4 and its Biological Activity as a Pro-Resolving Lipid Mediator of Neuroinflammation.立体控制全合成脂氧素 B4 及其作为神经炎症促解决脂质介质的生物学活性。
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本文引用的文献

1
Aspirin-triggered 15-epi-lipoxin A4 (LXA4) and LXA4 stable analogues are potent inhibitors of acute inflammation: evidence for anti-inflammatory receptors.阿司匹林触发的15-表-脂氧素A4(LXA4)和LXA4稳定类似物是急性炎症的有效抑制剂:抗炎受体的证据。
J Exp Med. 1997 May 5;185(9):1693-704. doi: 10.1084/jem.185.9.1693.
2
Lipoxins and novel aspirin-triggered 15-epi-lipoxins (ATL): a jungle of cell-cell interactions or a therapeutic opportunity?脂氧素与新型阿司匹林触发的15-表-脂氧素(ATL):细胞间相互作用的复杂局面还是治疗契机?
Prostaglandins. 1997 Feb;53(2):107-37. doi: 10.1016/s0090-6980(97)00001-4.
3
Lipoxin A4 inhibits cholinergic neurotransmission through nitric oxide generation in the rabbit trachea.脂氧素A4通过兔气管中一氧化氮的生成来抑制胆碱能神经传递。
Eur J Pharmacol. 1995 Dec 20;287(3):233-8. doi: 10.1016/0014-2999(95)00490-4.
4
Lipoxin A4 and B4 inhibit leukotriene-stimulated interactions of human neutrophils and endothelial cells.脂氧素A4和B4可抑制白三烯刺激的人中性粒细胞与内皮细胞的相互作用。
J Immunol. 1996 Mar 15;156(6):2264-72.
5
Lipoxin A4 modulates transmigration of human neutrophils across intestinal epithelial monolayers.脂氧素A4调节人中性粒细胞跨肠上皮单层的迁移。
J Clin Invest. 1993 Jul;92(1):75-82. doi: 10.1172/JCI116601.
6
Mechanisms of neutrophil-dependent and neutrophil-independent endothelial cell injury.中性粒细胞依赖性和非依赖性内皮细胞损伤的机制。
Biol Signals. 1994 Jan-Feb;3(1):1-14. doi: 10.1159/000109521.
7
Microvascular mechanisms in inflammation.炎症中的微血管机制。
Adv Prostaglandin Thromboxane Leukot Res. 1994;22:91-9.
8
Design of lipoxin A4 stable analogs that block transmigration and adhesion of human neutrophils.阻断人中性粒细胞迁移和黏附的脂氧素A4稳定类似物的设计
Biochemistry. 1995 Nov 7;34(44):14609-15. doi: 10.1021/bi00044a041.
9
Lipoxin A4 and lipoxin B4 inhibit chemotactic responses of human neutrophils stimulated by leukotriene B4 and N-formyl-L-methionyl-L-leucyl-L-phenylalanine.脂氧素A4和脂氧素B4可抑制白三烯B4和N-甲酰-L-甲硫氨酰-L-亮氨酰-L-苯丙氨酸刺激的人中性粒细胞的趋化反应。
Clin Sci (Lond). 1989 Aug;77(2):195-203. doi: 10.1042/cs0770195.
10
Biosynthesis and biological activity of leukotriene B4.白三烯B4的生物合成与生物活性
Clin Biochem. 1990 Oct;23(5):459-68. doi: 10.1016/0009-9120(90)90272-v.

局部应用阿司匹林触发的15-表-脂氧素A4和新型脂氧素B4稳定类似物可抑制中性粒细胞介导的血管通透性变化。

Neutrophil-mediated changes in vascular permeability are inhibited by topical application of aspirin-triggered 15-epi-lipoxin A4 and novel lipoxin B4 stable analogues.

作者信息

Takano T, Clish C B, Gronert K, Petasis N, Serhan C N

机构信息

Center for Experimental Therapeutics and Reperfusion Injury, Department of Anesthesia, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

J Clin Invest. 1998 Feb 15;101(4):819-26. doi: 10.1172/JCI1578.

DOI:10.1172/JCI1578
PMID:9466977
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC508630/
Abstract

Neutrophil (PMN) activation is critical in inflammation and reperfusion injury, suggesting that PMN-directed therapies may be of clinical use. Here, leukotriene B4 (LTB4)-induced PMN influx in ear skin was equivalent between 5-lipoxygenase knockout and wild-type mice. To explore actions of lipoxin (LX) in PMN-mediated tissue injury, we prepared several novel LX stable analogues, including analogues of LXA4 and aspirin-triggered 15-epi-LXA4 as well as LXB4, and examined their impact in PMN infiltration and vascular permeability. Each applied topically to mouse ears inhibited dramatically PMN-mediated increases in vascular permeability (IC50 range of 13-26 nmol) with a rank order of 15(R/S)-methyl-LXA4 > 16-para-fluoro-phenoxy-LXA4 approximately 5(S)-methyl-LXB4 >/= 16-phenoxy-LXA4 > 5(R)-methyl-LXB4. These LX mimetics were as potent as an LTB4 receptor antagonist, yet results from microphysiometry with mouse leukocytes indicated that they do not act as LTB4 receptor level antagonists. In addition, within 24 h of delivery, > 90% were cleared from ear biopsies. Neither IL-8, FMLP, C5a, LTD4, nor platelet-activating factor act topically to promote PMN influx. When applied with LTB4, PGE2 enhanced sharply both infiltration and vascular permeability, which were inhibited by a fluorinated stable analogue of aspirin-triggered LX. These results indicate that mimetics of LXs and aspirin-triggered 15-epi-LXA4 are topically active in this model and are potent inhibitors of both PMN infiltration and PMN-mediated vascular injury.

摘要

中性粒细胞(PMN)的激活在炎症和再灌注损伤中至关重要,这表明针对PMN的治疗方法可能具有临床应用价值。在此,白三烯B4(LTB4)诱导的耳部皮肤PMN流入在5-脂氧合酶基因敲除小鼠和野生型小鼠之间相当。为了探究脂氧素(LX)在PMN介导的组织损伤中的作用,我们制备了几种新型的LX稳定类似物,包括LXA4和阿司匹林触发的15-表-LXA4以及LXB4的类似物,并研究了它们对PMN浸润和血管通透性的影响。将每种类似物局部应用于小鼠耳部,均能显著抑制PMN介导的血管通透性增加(IC50范围为13 - 26 nmol),其活性顺序为15(R/S)-甲基-LXA4 > 16-对氟苯氧基-LXA4 ≈ 5(S)-甲基-LXB4 ≥ 16-苯氧基-LXA4 > 5(R)-甲基-LXB4。这些LX模拟物与LTB4受体拮抗剂一样有效,但小鼠白细胞微流控分析结果表明它们并非作为LTB4受体水平的拮抗剂起作用。此外,在给药后24小时内,超过90%的类似物从耳部活检组织中清除。白细胞介素-8、N-甲酰甲硫氨酸-亮氨酸-苯丙氨酸、C5a、白三烯D4以及血小板活化因子局部应用均不能促进PMN流入。当与LTB4一起应用时,前列腺素E2会急剧增强浸润和血管通透性,而阿司匹林触发的LX的氟化稳定类似物可抑制这种增强作用。这些结果表明,LX和阿司匹林触发的15-表-LXA4的模拟物在该模型中具有局部活性,并且是PMN浸润和PMN介导的血管损伤的有效抑制剂。