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细胞因子对源自小鼠骨髓和外周血单个核细胞的肥大细胞的不同作用的证明。

Demonstration of differential effects of cytokines on mast cells derived from murine bone marrow and peripheral blood mononuclear cells.

作者信息

Rottem M, Hull G, Metcalfe D D

机构信息

Allergic Diseases Section, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892.

出版信息

Exp Hematol. 1994 Nov;22(12):1147-55.

PMID:7523167
Abstract

Mouse bone marrow (BM) was cultured in the presence of recombinant mouse (rm) interleukin-3 (IL-3), rmIL-4, rmIL-5, rmIL-7, purified mouse (m) IL-9, rmIL-10, recombinant human (rh) macrophage-colony-stimulating factors (M-CSF), rm granulocyte-macrophage colony-stimulating factors (GM-CSF) rm stem cell factor (SCF), rh interferon-alpha (IFN-alpha), rmIFN-gamma, and mNGF to determine which cytokine would give rise to mast cells in murine BM cultures. From a starting population of 1 x 10(7) cells, 1.55 x 10(7) mast cells developed within 14 days in cultures supplemented by rmIL-3. No mast cells were seen at day 14 when any of the other cytokines were present alone, except for rmSCF, which supported the growth of < 0.01% of mast cells observed in IL-3-dependent BM cultures. When rmIL-4, -5, -7, -10, mIL-9, rhM-CSF, rmGM-CSF, rmSCF, rhIFN-alpha, -gamma, or mNGF were added to BM cultures in the presence of rmIL-3, mast cell growth increased 200% with the addition of rmSCF, and 10% when rmIL-4 or IL-9 was added. However, the addition of rhM-CSF, rmGM-CSF, rmIFN-gamma, and mNGF decreased the number of mast cells. Mast cell number, as determined by metachromatic stains, generally approximated the number of Fc epsilon RI+ cells as assessed by FACS analysis. Among the cytokines, only rmIL-4 and rmSCF were able to support the survival of mast cell progenitors in the absence of obvious mast cell proliferation, similarly to rmIL-3. Only rmSCF alone, or in combination with rmIL-3 or -4, supported the growth of mast cells from mouse peripheral blood mononuclear cells (PBMC) where the number of mast cell precursors was about 90 per 10(6) PBMC. With time, mouse BM cells cultured in rmIL-3 became more responsive to rmSCF. Taken together, these data demonstrate that IL-3 is a major early mast cell growth factor, that mast cells become more dependent on SCF with time, and that the effects of IL-3 and SCF are upregulated (IL-4) or downregulated (M-CSF, GM-CSF, IFN-gamma) by both growth factors and proinflammatory cytokines.

摘要

在重组小鼠(rm)白细胞介素-3(IL-3)、rmIL-4、rmIL-5、rmIL-7、纯化的小鼠(m)IL-9、rmIL-10、重组人(rh)巨噬细胞集落刺激因子(M-CSF)、rm粒细胞-巨噬细胞集落刺激因子(GM-CSF)、rm干细胞因子(SCF)、rh干扰素-α(IFN-α)、rmIFN-γ和mNGF存在的情况下培养小鼠骨髓(BM),以确定哪种细胞因子会在小鼠BM培养物中产生肥大细胞。从1×10⁷个细胞的起始群体开始,在补充rmIL-3的培养物中,14天内产生了1.55×10⁷个肥大细胞。当单独存在任何其他细胞因子时,在第14天未观察到肥大细胞,除了rmSCF,其支持的肥大细胞生长在依赖IL-3的BM培养物中观察到的不到0.01%。当在rmIL-3存在的情况下将rmIL-4、-5、-7、-10、mIL-9、rhM-CSF、rmGM-CSF、rmSCF、rhIFN-α、-γ或mNGF添加到BM培养物中时,添加rmSCF后肥大细胞生长增加200%,添加rmIL-4或IL-9时增加10%。然而,添加rhM-CSF, rmGM-CSF, rmIFN-γ和mNGF会减少肥大细胞的数量。通过异染性染色确定的肥大细胞数量通常与通过FACS分析评估的FcεRI⁺细胞数量相近。在这些细胞因子中,只有rmIL-4和rmSCF能够在没有明显肥大细胞增殖的情况下支持肥大细胞祖细胞的存活,与rmIL-3类似。只有单独的rmSCF,或与rmIL-3或-4联合使用,才能支持从小鼠外周血单个核细胞(PBMC)中生长肥大细胞,其中肥大细胞前体的数量约为每10⁶个PBMC中有90个。随着时间的推移,在rmIL-3中培养的小鼠BM细胞对rmSCF的反应性增强。综上所述,这些数据表明IL-3是主要的早期肥大细胞生长因子,肥大细胞随着时间的推移对SCF的依赖性增加,并且IL-3和SCF的作用会被生长因子和促炎细胞因子上调(IL-4)或下调(M-CSF、GM-CSF、IFN-γ)。

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