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白三烯B4是与克隆的趋化因子受体CMKRL1结合并激活该受体的功能性配体。

Leukotriene B4 is the functional ligand binding to and activating the cloned chemoattractant receptor, CMKRL1.

作者信息

Owman C, Sabirsh A, Boketoft A, Olde B

机构信息

Department of Physiology and Neuroscience, Wallenberg Neuroscience Center, University of Lund, Sweden.

出版信息

Biochem Biophys Res Commun. 1997 Nov 7;240(1):162-6. doi: 10.1006/bbrc.1997.7628.

Abstract

We recently described a novel chemoattractant receptor, provisionally named CMKRL1, which has turned out to be the first cloned leukotriene (LT) receptor. Present binding assays using tritiated LTB4 and isolated membranes from COS-7 cells, transiently transfected with cDNA encoding this receptor, yielded a linear Scatchard plot showing expression of only a single, high-affinity receptor population with a mean Kd of 2.1 nM and Bmax of 17.0 pmoles/mg protein. Sham-transfected cells exhibited no specific binding. LTB4 elicited concentration-dependent increases in intracellular calcium measured with Fura-2 in individual CHO cells stably expressing CMKRL1. No response was seen with sham-transfected control cells, or in calcium-free medium which suggests that calcium mainly originates from extracellular sources. The LTB4-induced cellular calcium increment was blocked in the presence of a monoclonal antibody, raised against a synthetic peptide corresponding to the extracellular tail of CMKRL1 and capable of visualizing the receptor by fluorescence immunocytochemistry. Taken together the analyses show that LTB4 is the endogenous ligand for CMKRL1 which is, thus, identical to the LTB4 receptor, designated BLTR according to the NC-IUPHAR nomenclature.

摘要

我们最近描述了一种新型趋化因子受体,暂命名为CMKRL1,结果它成为首个克隆的白三烯(LT)受体。使用氚标记的LTB4和从瞬时转染了编码该受体的cDNA的COS-7细胞分离的膜进行的现有结合试验,得到了一条线性Scatchard图,显示仅表达单一的高亲和力受体群体,平均Kd为2.1 nM,Bmax为17.0 pmoles/mg蛋白质。假转染细胞未表现出特异性结合。在稳定表达CMKRL1的单个CHO细胞中,用Fura-2测量发现LTB4引起细胞内钙浓度依赖性增加。假转染的对照细胞或无钙培养基中未观察到反应,这表明钙主要来源于细胞外。在存在针对与CMKRL1细胞外尾相对应的合成肽产生的单克隆抗体的情况下,LTB4诱导的细胞钙增加被阻断,该单克隆抗体能够通过荧光免疫细胞化学使受体可视化。综合分析表明,LTB4是CMKRL1的内源性配体,因此,CMKRL1与LTB4受体相同,根据NC-IUPHAR命名法命名为BLTR。

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