Ryan J J, Kinzer C A, Paul W E
Laboratory of Immunology, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland 20892-1892, USA.
J Exp Med. 1995 Aug 1;182(2):567-74. doi: 10.1084/jem.182.2.567.
A population of cells that express mast cell markers, including the membrane protein p161, but that lack expression of the high affinity IgE receptor, Fc epsilon RI, can be routinely grown from bone marrow. Ionomycin, but not IgE immune complexes, causes these cells to release serotonin and to express IL-3 and IL-13 mRNA, consistent with their being FC epsilon RI-deficient mast cells. These p161+/Fc epsilon RI- mast cells expressed normal amounts of Fc epsilon RI alpha and beta chain mRNA, but extremely low levels of Fc epsilon RI gamma chain mRNA. In addition, this novel mast cell population expressed CD3 zeta chain mRNA, which p161+/Fc epsilon RI+ mast cells did not. CD3 zeta stable transfectants of Abelson-murine leukemia virus-transformed p161+/Fc epsilon RI+ mast cells continued to express Fc epsilon RI. This strongly suggests that the failure of p161+/Fc epsilon RI- mast cells to express IgE receptors was not caused by the presence of CD3 zeta chain. Transfection of human Fc epsilon RI gamma cDNA into p161+/Fc epsilon RI- mast cells rescued IgE binding. These stable transfectants released serotonin in response to cross-linkage of Fc epsilon RI, demonstrating that the molecular defect of p161+/Fc epsilon RI- mast cells is indeed the loss of Fc epsilon RI gamma expression.
一群表达肥大细胞标志物(包括膜蛋白p161)但缺乏高亲和力IgE受体FcεRI表达的细胞可常规地从骨髓中培养出来。离子霉素而非IgE免疫复合物可使这些细胞释放5-羟色胺并表达IL-3和IL-13 mRNA,这与其作为FcεRI缺陷型肥大细胞相一致。这些p161+/FcεRI-肥大细胞表达正常量的FcεRIα和β链mRNA,但FcεRIγ链mRNA水平极低。此外,这种新型肥大细胞群体表达CD3ζ链mRNA,而p161+/FcεRI+肥大细胞则不表达。阿贝尔逊鼠白血病病毒转化的p161+/FcεRI+肥大细胞的CD3ζ稳定转染子继续表达FcεRI。这强烈表明p161+/FcεRI-肥大细胞未能表达IgE受体并非由CD3ζ链的存在所致。将人FcεRIγ cDNA转染到p161+/FcεRI-肥大细胞中可挽救IgE结合。这些稳定转染子在FcεRI交联时释放5-羟色胺,表明p161+/FcεRI-肥大细胞的分子缺陷确实是FcεRIγ表达缺失。
