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跨膜信号传导:一种由复合Fc受体介导的信号转导的离子通量非依赖模型。

Transmembrane signaling: an ion-flux-independent model for signal transduction by complexed Fc receptors.

作者信息

Pfefferkorn L C

出版信息

J Cell Biol. 1984 Dec;99(6):2231-40. doi: 10.1083/jcb.99.6.2231.

Abstract

Fluxes of Na+/K+ that precede effector functions in stimulated phagocytes are thought to play a role in signal transduction. To examine this hypothesis, phagocytosis, phagosomal acidification, and superoxide anion generation (O2-) were stimulated in media in which the Na+ was replaced with K+ or choline+. Counts of particles internalized and assessment of acidification of the phagosomes by acridine orange staining indicated that Na+/K+ fluxes were not necessary for phagocytosis or phagosomal acidification in J774.2 macrophages. Phagocytosis mediated by the ionophoretic Fc receptor gamma 2b/gamma 1 of J774.2 macrophages was equally independent of a Na+ gradient. Na+/K+ fluxes did not dictate the rate of O2- generation in human monocytes. Therefore, in at least these three effector functions, Na+/K+ fluxes stimulated by Fc- and non-specific receptor binding play neither a signaling nor an enhancing role. An ion-flux-independent model for transmembrane signaling by the Fc receptor is proposed. Others have shown that there is an apparent dependence on the external Na+ concentration for O2- generation and lysosomal secretion by neutrophils. These neutrophils had been pre-treated with NH4+ during a routine purification step. O2- generation stimulated by opsonized zymosan or phorbol myristate acetate, by monocytes or monocyte-derived macrophages, and phagocytosis of opsonized zymosan by J774.2 macrophages, showed dependence on external Na+ only if these cells had been pre-treated with NH4+. Brief NH4+ pre-treatment would be expected to acidify the cytoplasm of the cells. The reversal of this acidification is known to require Na+ for H+ extrusion through the Na+/H+ antiport, thus explaining the apparent Na+ dependence.

摘要

在受刺激的吞噬细胞中,效应功能之前的Na⁺/K⁺通量被认为在信号转导中起作用。为了检验这一假设,在Na⁺被K⁺或胆碱⁺替代的培养基中刺激吞噬作用、吞噬体酸化和超氧阴离子生成(O₂⁻)。通过吖啶橙染色对内化颗粒的计数以及对吞噬体酸化的评估表明,在J774.2巨噬细胞中,吞噬作用或吞噬体酸化并不需要Na⁺/K⁺通量。J774.2巨噬细胞的离子载体Fc受体γ2b/γ1介导的吞噬作用同样不依赖于Na⁺梯度。Na⁺/K⁺通量并不决定人类单核细胞中O₂⁻的生成速率。因此,至少在这三种效应功能中,由Fc和非特异性受体结合刺激的Na⁺/K⁺通量既不发挥信号作用也不发挥增强作用。提出了一种Fc受体跨膜信号传导的离子通量非依赖性模型。其他人已经表明,中性粒细胞的O₂⁻生成和溶酶体分泌明显依赖于外部Na⁺浓度。这些中性粒细胞在常规纯化步骤中用NH₄⁺进行了预处理。仅当这些细胞用NH₄⁺预处理时,调理酵母聚糖或佛波酯肉豆蔻酸酯刺激的O₂⁻生成、单核细胞或单核细胞衍生巨噬细胞的O₂⁻生成以及J774.2巨噬细胞对调理酵母聚糖的吞噬作用才显示出对外部Na⁺的依赖性。短暂的NH₄⁺预处理预计会使细胞的细胞质酸化。已知这种酸化的逆转需要Na⁺通过Na⁺/H⁺反向转运体排出H⁺,从而解释了明显的Na⁺依赖性。

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