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The Efficacy of the Novel TSPO Ligands 2-Cl-MGV-1 and 24-Di-Cl-MGV-1 Compared to the Classical TSPO Ligand PK 11195 to Counteract the Release of Chemokines from LPS-Stimulated BV-2 Microglial Cells

机译：与经典TSPO配体PK 11195相比新型TSPO配体2-C1-MGV-1和24-DI-CL-MGV-1的功效与LPS刺激的BV-2微胶质细胞抵消了趋化因子的释放

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The impact of ligands of the 18 kDa translocator protein (TSPO) on the release of chemokines is not vastly investigated. In the present study, we assessed the effect of our novel TSPO ligands 2-Cl-MGV-1 and 2,4-Di-Cl-MGV-1 compared to the classical TSPO ligand PK 11195 on chemokine release in LPS-stimulated BV-2 microglial cells. As per the effect of 2-Cl-MGV-1, CCL2, CCL3, and CCL5 were inhibited by 90%, CCL8 by 97%, and IL-2 by 77% (p < 0.05 for all). 2,4-Di-Cl-MGV-1 inhibited CCL2 release by 92%, CCL3 by 91%, CCL5 by 90%, CCL8 by 89%, and IL-2 by 80% (p < 0.05 for all). PK 11195 exhibited weaker inhibitory effects: CCL2 by 22%, CCL3 by 83%, CCL5 by 34%, CCL8 by 41%, and the cytokine IL-2 by 14% (p < 0.05 for all). Thus, it appears that the novel TSPO ligands are potent suppressors of LPS-stimulated BV-2 microglial cells, and their inhibitory effect is larger than that of PK 11195. Such immunomodulatory effects on microglial cells may be relevant to the treatment of neurodegenerative and neuroinflammatory diseases.

机译：18kDa易位蛋白（TSPO）对趋化因子释放的联合体的影响不会大大研究。在本研究中，与LPS刺激的BV-中的趋化因子释放的经典TSPO配体PK 11195相比，评估了我们的新型TSPO配体2-C1-MGV-1和2,4-DI-CL-MGV-1的效果。 2个小胶质细胞。根据2-Cl-Mgv-1，CCl2，CCl3和CCl5的影响，将90％，CCl8抑制97％，IL-2抑制77％（所有P <0.05）。将2,4-Di-Cl-MgV-1抑制CCl2释放92％，CCl3释放91％，CCl5×90％，CCl8×89％，均为80％（P <0.05）。 PK 11195表现出较弱的抑制作用：CCl2×22％，CCl3×83％，CCl5×34％，CCl8×41％，细胞因子IL-2×14％（全部为P <0.05）。因此，新型Tspo配体是LPS刺激的BV-2微胶质细胞的有效抑制剂，它们的抑制作用大于PK 11195的抑制作用。这些对微胶质细胞的免疫调节作用可能与神经变性和神经炎症的治疗相关疾病。

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期刊名称 Biology
作者
Sheelu Monga; Abraham Weizman; Moshe Gavish;
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作者单位

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年(卷),期 2020(9),9
年度 2020
页码 291
总页数 8
原文格式 PDF
正文语种
中图分类生物学;
关键词
chemokines; CCL; IL-2; microglia; inflammation; TSPO;

机译：趋化因子;CCL;IL-2;小胶质细胞;炎症;TSPO;

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1. Inhibitory Effects of the Two Novel TSPO Ligands 2-Cl-MGV-1 and MGV-1 on LPS-induced Microglial Activation [J] . Sheelu Monga, Rafi Nagler, Rula Amara, Cells . 2019,第5期

机译：两种新型TSPO配体2-Cl-MgV-1和MGV-1对LPS诱导的微胶质活化的抑制作用
2. The translocator protein (TSPO) ligand PK11195 induces apoptosis and cell cycle arrest and sensitizes to chemotherapy treatment in pre- and post-relapse neuroblastoma cell lines [J] . Mendon?a-TorresM.C., RobertsS.S. Cancer biology & therapy . 2013,第4期

机译：转运蛋白（TSPO）配体PK11195诱导凋亡和细胞周期停滞，并对复发前和复发后神经母细胞瘤细胞系的化学疗法敏感
3. In vitro mitochondrial effects of PK 11195, a synthetic translocator protein 18 kDa (TSPO) ligand, in human osteoblast-like cells [J] . Rosenberg N., Rosenberg O., Weizman A., Journal of Bioenergetics and Biomembranes . 2011,第6期

机译：PK 11195（一种合成的转运蛋白18 kDa（TSPO）配体）在人成骨细胞样细胞中的体外线粒体作用
4. The TSPO Ligands 2-Cl-MGV-1 MGV-1 and PK11195 Differentially Suppress the Inflammatory Response of BV-2 Microglial Cell to LPS [O] . Maya Azrad, Nidal Zeineh, Abraham Weizman, 2019

机译：TSPO配体2-Cl-MGV-1MGV-1和PK11195差异性抑制BV-2小胶质细胞对LPS的炎症反应
5. The Efficacy of the Novel TSPO Ligands 2-Cl-MGV-1 and 2,4-Di-Cl-MGV-1 Compared to the Classical TSPO Ligand PK 11195 to Counteract the Release of Chemokines from LPS-Stimulated BV-2 Microglial Cells [O] . Sheelu Monga, Abraham Weizman, Moshe Gavish 2020

机译：与经典TSPO配体PK 11195相比，新型TSPO配体2-C1-MGV-1和2,4-DI-CL-MGV-1的功效与LPS刺激的BV-2微胶质细胞抵消了趋化因子的释放

The Efficacy of the Novel TSPO Ligands 2-Cl-MGV-1 and 24-Di-Cl-MGV-1 Compared to the Classical TSPO Ligand PK 11195 to Counteract the Release of Chemokines from LPS-Stimulated BV-2 Microglial Cells

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