溶血磷脂通过增加肝素结合表皮生长因子的表达增强人T细胞对白喉毒素的敏感性。

E J Goetzl, Y Kong, J S Kenney
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引用次数: 19

摘要

本文研究了溶血磷脂酸(LPA)和鞘氨醇1-磷酸(S1P)对人CD4+ 8+ 3low T淋巴母细胞瘤tsup1培养细胞株中白喉毒素受体肝素结合表皮生长因子样生长因子(HB-EGF) T细胞表达的影响。Tsup-1细胞携带内皮分化基因(edg)-2和-4编码的G蛋白偶联受体(gpcr),用于LPA, edg -3和-5编码的gpcr用于S1P。LPA和S1P增强了DT对Tsup-1细胞蛋白合成的抑制作用,其脂质结构特异性与Edg受体识别所需的脂质结构特异性相似。LPA和S1P可提高Tsup-1细胞中HB-EGF的免疫反应水平,而HB-EGF中和抗体可抑制LPA和S1P增强Tsup-1细胞对DT的敏感性。用编码Edg-2 + -4反义mRNA的质粒组合稳定转染tsp -1细胞,在Western blot中抑制了Edg-2和-4的水平,但没有抑制Edg-3和-5的水平,并平行降低了LPA引起的HB-EGF的增加和对DT的敏感性,而不是S1P。同样转染Edg-3 + -5反义质粒可抑制Tsup-1细胞中Edg-3和-5的免疫反应水平,但对Edg-2和-4无抑制作用,同时降低S1P-,但不降低LPA-,诱导Tsup-1细胞中HB-EGF和DT易感性均增加。因此,Edg gpcr介导的LPA和S1P增强T细胞对DT的敏感性可能归因于DT受体HB-EGF的表达增加。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Lysophospholipid enhancement of human T cell sensitivity to diphtheria toxin by increased expression of heparin-binding epidermal growth factor.

The effects of lysophosphatidic acid (LPA) and sphingosine 1-phosphate (S1P) on T cell expression of heparin-binding epidermal growth factor-like growth factor (HB-EGF), the diphtheria toxin (DT) receptor, were investigated in the Tsup-1 cultured line of human CD4+ 8+ 3low T lymphoblastoma cells. Tsup-1 cells bear endothelial differentiation gene (edg)-2 and -4-encoded G protein-coupled receptors (GPCRs) for LPA and Edg-3 and -5 GPCRs for S1P. Suppression by DT of Tsup-1 cell protein synthesis was enhanced by LPA and S1P, with lipid structural specificity similar to that required for their recognition by Edg receptors. LPA and S1P increased the Tsup-1 cell level of immunoreactive HB-EGF, and neutralizing antibodies to HB-EGF inhibited LPA and S1P enhancement of Tsup-1 cell susceptibility to DT. Stabilized transfection of Tsup-1 cells with a combination of plasmids encoding Edg-2 plus -4 antisense mRNA suppressed the levels of Edg-2 and -4, but not Edg-3 and -5, in Western blots and reduced in parallel the increments in HB-EGF and susceptibility to DT evoked by LPA but not S1P. Similar transfection with Edg-3 plus -5 antisense plasmids suppressed Tsup-1 cell levels of immunoreactive Edg-3 and -5, but not Edg-2 or -4, and concurrently reduced S1P-, but not LPA-, induced Tsup-1 cell increases in both HB-EGF and susceptibility to DT. Edg GPCR-mediated LPA and S1P enhancement of T cell sensitivity to DT, thus, may be attributable to increased expression of the DT receptor HB-EGF.

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