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首页> 外文期刊>The journal of immunology >Use of a Photoactivatable Taxol Analogue to Identify Unique Cellular Targets in Murine Macrophages: Identification of Murine CD18 as a Major Taxol-Binding Protein and a Role for Mac-1 in Taxol-Induced Gene Expression
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Use of a Photoactivatable Taxol Analogue to Identify Unique Cellular Targets in Murine Macrophages: Identification of Murine CD18 as a Major Taxol-Binding Protein and a Role for Mac-1 in Taxol-Induced Gene Expression

机译:使用可光活化紫杉醇类似物来鉴定小鼠巨噬细胞中的独特细胞靶标:鉴定作为主要紫杉醇结合蛋白的小鼠CD18和Mac-1在紫杉醇诱导的基因表达中的作用

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Taxol, a potent antitumor agent that binds β-tubulin and promotes microtubule assembly, results in mitotic arrest at the G2/M phase of the cell cycle. More recently, Taxol was shown to be a potent LPS mimetic in murine, but not in human macrophages, stimulating signaling pathways and gene expression indistinguishably from LPS. Although structurally unrelated to LPS, Taxol’s LPS-mimetic activities are blocked by inactive structural analogues of LPS, indicating that despite the species-restricted effects of Taxol, LPS and Taxol share a common receptor/signaling complex that might be important in LPS-induced human diseases. To identify components of the putatively shared Taxol/LPS receptor, a novel, photoactivatable Taxol analogue was employed to identify unique Taxol-binding proteins in murine macrophage membranes. Seven major Taxol-binding proteins, ranging from ~50 to 200 kDa, were detected. Although photoactivatable Taxol analogue failed to bind to CD14, the prominent Taxol-binding protein was identified as CD18, the ~96-kDa common component of the β2 integrin family. This finding was supported by the concomitant failure of macrophage membranes from Mac-1 knockout mice to express immunoreactive CD18 and the major Taxol-binding protein. In addition, Taxol-induced IL-12 p40 mRNA was markedly reduced in Mac-1 knockout macrophages and anti-Mac-1 Ab blocked secretion of IL-12 p70 in Taxol- and LPS-stimulated macrophages. Since CD18 has been described as a participant in LPS-induced binding and signal transduction, these data support the hypothesis that the interaction of murine CD18 with Taxol is involved in its proinflammatory activity.
机译:紫杉醇是一种有效的抗肿瘤剂,可结合β-微管蛋白并促进微管组装,可导致细胞周期G2 / M期的有丝分裂停滞。最近,紫杉醇在鼠类中被证明是有效的LPS模仿物,但在人类巨噬细胞中却不然,刺激信号通路和基因表达与LPS毫无区别。尽管在结构上与LPS不相关,但紫杉醇的LPS模拟活性被LPS的非活性结构类似物阻断,这表明尽管紫杉醇具有物种限制作用,但LPS和紫杉醇具有共同的受体/信号复合物,这对LPS诱导的人类可能很重要疾病。为了鉴定假定共有的紫杉醇/ LPS受体的成分,采用了一种新型的,可光活化的紫杉醇类似物来鉴定鼠巨噬细胞膜中独特的紫杉醇结合蛋白。检测到7种主要的紫杉醇结合蛋白,范围从〜50到200 kDa。尽管可光活化的紫杉醇类似物未能与CD14结合,但著名的紫杉醇结合蛋白被鉴定为CD18,它是β2整联蛋白家族的〜96-kDa共同成分。这项发现得到了Mac-1基因敲除小鼠巨噬细胞膜同时表达免疫反应性CD18和主要紫杉醇结合蛋白的支持。此外,紫杉醇诱导的IL-12 p40 mRNA在Mac-1敲除巨噬细胞中显着减少,而抗Mac-1 Ab阻止了紫杉醇和LPS刺激的巨噬细胞IL-12 p70的分泌。由于CD18被描述为LPS诱导的结合和信号转导的参与者,因此这些数据支持以下假设,即鼠CD18与紫杉醇的相互作用参与其促炎活性。

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