Identification of two novel LPS-binding proteins in Kupffer cells: implications in TNF-α production

P. Thomas, D. Lazure, R. Moussa, O. Bajenova, P. Burke, A. Ganguly, R. Armour Forse
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引用次数: 8

Abstract

Using a combination of gel-exclusion chromatography and ligand binding with [125I]-lipopolysaccharide (LPS), we discovered two novel endotoxin-binding proteins, p31LPB and p34LPB, in Kupffer cells. Their molecular masses suggest that these are previously undescribed LPS-binding proteins (LBPs). Evidence from detergent-based cell extractions shows that these proteins are probably transmembrane or located on the inner leaflet of the lipid bilayer. We have partially purified the proteins from detergent extracts of Kupffer cells and proven that they bind diphosphoryl lipid A, an interaction associated with TNF-α production. The proteins do not bind monophosphoryl lipid A. Diphosphoryl lipid A binding occurs in the absence of serum, suggesting a mechanism of cytokine production distinct from that involving CD14 and lipopolysaccharide-binding protein (LPB). The two proteins were not detectable in resident peritoneal macrophages or in a number of other cell lines of the macrophage/monocyte lineage, suggesting specificity towards terminally differentiated macrophages such as Kupffer cells.
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在Kupffer细胞中鉴定两种新的lps结合蛋白:对TNF-α产生的影响
采用凝胶排斥层析和配体结合[125I]-脂多糖(LPS)的方法,我们在Kupffer细胞中发现了两种新的内毒素结合蛋白p31LPB和p34LPB。它们的分子质量表明它们是以前未描述过的脂多糖结合蛋白(lbp)。基于洗涤剂的细胞提取证据表明,这些蛋白质可能是跨膜的或位于脂质双分子层的内小叶。我们已经从Kupffer细胞的洗涤剂提取物中部分纯化了蛋白质,并证明它们与二磷酰脂质A结合,这是与TNF-α产生相关的相互作用。这些蛋白不结合单磷酰脂质A。二磷酰脂质A的结合发生在没有血清的情况下,这表明细胞因子的产生机制不同于涉及CD14和脂多糖结合蛋白(LPB)的机制。这两种蛋白在腹膜巨噬细胞或巨噬细胞/单核细胞谱系的许多其他细胞系中均未检测到,提示对终分化巨噬细胞(如Kupffer细胞)具有特异性。
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