Columbo M, Horowitz E M, Botana L M, MacGlashan D W, Bochner B S, Gillis S, Zsebo K M, Galli S J, Lichtenstein L M
Department of Medicine, Johns Hopkins University School of Medicine, Johns Hopkins Asthma and Allergy Center, Baltimore, MD 21224.
J Immunol. 1992 Jul 15;149(2):599-608.
The gene product of the steel locus of the mouse represents a growth factor for murine mast cells and a ligand for the c-kit proto-oncogene receptor, a member of the tyrosine kinase receptor class of oncogenes (for review, see O. N. Witte. 1990. Cell 63:5). We have studied the effect of the human recombinant c-kit receptor ligand stem cell factor (rhSCF) on the release of inflammatory mediators from human skin mast cells and peripheral blood basophils and compared its activity to that of rhIL-3, rhSCF (1 ng/ml to 1 microgram/ml) activated the release of histamine and PGD2 from mast cells isolated from human skin. Analysis by digital video microscopy indicated that purified human skin mast cells (84 +/- 5% pure) responded to rhSCF (0.1 to 1 microgram/ml) challenge with a rapid, sustained rise in intracellular Ca2+ levels that was accompanied by secretion of histamine. A brief preincubation (10 min) of mast cells with rhSCF (0.1 pg/ml to 1 ng/ml) significantly enhanced (100 +/- 35%) the release of histamine induced by anti-IgE (3 micrograms/ml), but was much less effective on IgE-mediated release of PGD2. In contrast, a short term incubation with rhSCF did not potentiate the secretion of histamine activated by substance P (5 microM). A 24-h incubation of mast cells with rhSCF did not affect the release of mediators induced by anti-IgE (3 micrograms/ml), probably due to receptor desensitization, rhSCF (1 ng/ml to 3 micrograms/ml) neither caused release of histamine or leukotriene C4 (LTC4) release from leukocytes of 14 donors, nor induced a rise in intracellular Ca2+ levels in purified (greater than 70%) basophils. Brief preincubation (10 min) of leukocytes with rhSCF (1 ng/ml to 3 micrograms/ml) caused an enhancement (69 +/- 11%) of anti-IgE-induced release of histamine that was significant at concentrations as low as 3 ng/ml (p less than 0.05), whereas it appeared less effective in potentiating IgE-mediated LTC4 release. In contrast, a prolonged incubation (24 h) with rhSCF (0.1 pg/ml to 100 ng/ml) did not enhance the release of histamine or LTC4 induced by anti-IgE (0.1 microgram/ml), whereas rhIL-3 (3 ng/ml) significantly potentiated the release of both mediators.(ABSTRACT TRUNCATED AT 400 WORDS)
小鼠钢位点的基因产物代表一种针对鼠肥大细胞的生长因子以及原癌基因c-kit受体的配体,c-kit受体是癌基因中酪氨酸激酶受体家族的成员之一(综述见O.N.威特,1990年,《细胞》63卷:5期)。我们研究了重组人c-kit受体配体干细胞因子(rhSCF)对人皮肤肥大细胞和外周血嗜碱性粒细胞释放炎症介质的影响,并将其活性与重组人白细胞介素-3(rhIL-3)的活性进行比较。rhSCF(1纳克/毫升至1微克/毫升)可激活从人皮肤分离出的肥大细胞释放组胺和前列腺素D2。数字视频显微镜分析表明,纯化的人皮肤肥大细胞(纯度为84±5%)对rhSCF(0.1至1微克/毫升)刺激的反应是细胞内钙离子水平迅速、持续升高,并伴有组胺分泌。肥大细胞与rhSCF(0.1皮克/毫升至1纳克/毫升)短暂预孵育(10分钟)可显著增强(100±35%)抗IgE(3微克/毫升)诱导的组胺释放,但对IgE介导的前列腺素D2释放的作用要小得多。相比之下,与rhSCF短期孵育并不能增强P物质(5微摩尔)激活的组胺分泌。肥大细胞与rhSCF孵育24小时不影响抗IgE(3微克/毫升)诱导的介质释放,可能是由于受体脱敏。rhSCF(1纳克/毫升至3微克/毫升)既不会导致14名供体白细胞释放组胺或白三烯C4(LTC4),也不会使纯化的(>70%)嗜碱性粒细胞内钙离子水平升高。白细胞与rhSCF(1纳克/毫升至3微克/毫升)短暂预孵育(10分钟)可增强(69±11%)抗IgE诱导的组胺释放,在低至3纳克/毫升的浓度下就有显著效果(p<0.05),而在增强IgE介导的LTC4释放方面似乎效果较差。相比之下,与rhSCF长时间孵育(24小时)(0.1皮克/毫升至100纳克/毫升)并不能增强抗IgE(0.1微克/毫升)诱导的组胺或LTC4释放,而rhIL-3(3纳克/毫升)可显著增强这两种介质的释放。(摘要截选至400字)
