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Binding of monoclonal antibody AA4 to gangliosides on rat basophilic leukemia cells produces changes similar to those seen with Fc epsilon receptor activation.单克隆抗体AA4与大鼠嗜碱性白血病细胞上神经节苷脂的结合产生的变化类似于Fcε受体激活时所观察到的变化。
J Cell Biol. 1992 Feb;116(3):635-46. doi: 10.1083/jcb.116.3.635.
2
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Monoclonal antibody AA4, which inhibits binding of IgE to high affinity receptors on rat basophilic leukemia cells, binds to novel alpha-galactosyl derivatives of ganglioside GD1b.
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Binding properties and histamine release in variants of rat basophilic leukemia cells with changes in the IgE receptor.
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Calcium homeostasis in intact lymphocytes: cytoplasmic free calcium monitored with a new, intracellularly trapped fluorescent indicator.完整淋巴细胞中的钙稳态:用一种新的细胞内捕获荧光指示剂监测细胞质游离钙。
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Ligand-induced association of surface immunoglobulin with the detergent-insoluble cytoskeletal matrix of the B lymphocyte.配体诱导表面免疫球蛋白与B淋巴细胞的去污剂不溶性细胞骨架基质结合。
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Phorbol myristate acetate stimulates microtubule and 10-nm filament extension and lysosome redistribution in mouse macrophages.佛波醇肉豆蔻酸酯乙酸盐刺激小鼠巨噬细胞中的微管和10纳米细丝伸展以及溶酶体重新分布。
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Calcium and histamine secretion from mast cells.肥大细胞分泌钙和组胺。
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A tumor promoter induces rapid and coordinated reorganization of actin and vinculin in cultured cells.肿瘤启动子可诱导培养细胞中肌动蛋白和纽蛋白快速且协调的重组。
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Variants of the rat basophilic leukemia cell line for the study of histamine release.用于研究组胺释放的大鼠嗜碱性白血病细胞系变体
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IgE-induced histamine release from rat basophilic leukemia cell lines: isolation of releasing and nonreleasing clones.IgE诱导大鼠嗜碱性白血病细胞系释放组胺:释放和不释放克隆的分离
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Calcium/phospholipid-dependent kinase recognizes sites in microtubule-associated protein 2 which are phosphorylated in living brain and are not accessible to other kinases.
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单克隆抗体AA4与大鼠嗜碱性白血病细胞上神经节苷脂的结合产生的变化类似于Fcε受体激活时所观察到的变化。

Binding of monoclonal antibody AA4 to gangliosides on rat basophilic leukemia cells produces changes similar to those seen with Fc epsilon receptor activation.

作者信息

Oliver C, Sahara N, Kitani S, Robbins A R, Mertz L M, Siraganian R P

机构信息

Laboratory of Immunology, National Institute of Dental Research, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

J Cell Biol. 1992 Feb;116(3):635-46. doi: 10.1083/jcb.116.3.635.

DOI:10.1083/jcb.116.3.635
PMID:1370498
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2289326/
Abstract

The mAb AA4 binds to novel derivatives of the ganglioside Gd1b on rat basophilic leukemia (RBL-2H3) cells. Some of the gangliosides are located close to the high affinity IgE receptor (Fc epsilon RI), and binding of mAb AA4 inhibits Fc epsilon RI-mediated histamine release. In the present study, mAb AA4 was found to bind exclusively to mast cells in all rat tissues examined. In vitro, within 1 min of mAb AA4 binding, the cells underwent striking morphologic changes. They lost their normal spindle shaped appearance, increased their ruffling, and spread over the surface of the culture dish. These changes were accompanied by a redistribution of the cytoskeletal elements, actin, tubulin, and vimentin, but only the actin was associated with the membrane ruffles. Binding of mAb AA4 also induces a rise in intracellular calcium, stimulates phosphatidyl inositol breakdown, and activates PKC. However, the extent of these changes was less than that observed when the cells were stimulated with antigen or antibody directed against the Fc epsilon RI. None of these changes associated with mAb AA4 binding were seen when the cells were exposed to nonspecific IgG, IgE, or four other anti-cell surface antibodies, nor were the changes induced by binding mAb AA4 at 4 degrees C or in the absence of extracellular calcium. Although mAb AA4 does not stimulate histamine release, it enhances the effect of the calcium ionophore A23187 mediated release. The morphological and biochemical effects produced by mAb AA4 are similar to those seen following activation of the cell through the IgE receptor. Therefore, the surface gangliosides which bind mAb AA4 may function in modulating secretory events.

摘要

单克隆抗体AA4可与大鼠嗜碱性白血病(RBL - 2H3)细胞上神经节苷脂Gd1b的新型衍生物结合。其中一些神经节苷脂靠近高亲和力IgE受体(FcεRI),单克隆抗体AA4的结合会抑制FcεRI介导的组胺释放。在本研究中,发现单克隆抗体AA4在所有检测的大鼠组织中仅与肥大细胞结合。在体外,单克隆抗体AA4结合细胞1分钟内,细胞就会发生显著的形态变化。它们失去了正常的纺锤形外观,褶皱增多,并在培养皿表面铺展。这些变化伴随着细胞骨架成分肌动蛋白、微管蛋白和波形蛋白的重新分布,但只有肌动蛋白与膜褶皱相关。单克隆抗体AA4的结合还会导致细胞内钙浓度升高,刺激磷脂酰肌醇分解,并激活蛋白激酶C。然而,这些变化的程度小于用抗原或针对FcεRI的抗体刺激细胞时观察到的程度。当细胞暴露于非特异性IgG、IgE或其他四种抗细胞表面抗体时,未观察到与单克隆抗体AA4结合相关的这些变化,在4℃或无细胞外钙的情况下,单克隆抗体AA4结合也不会诱导这些变化。尽管单克隆抗体AA4不会刺激组胺释放,但它会增强钙离子载体A23187介导的释放作用。单克隆抗体AA4产生的形态学和生化效应与通过IgE受体激活细胞后观察到的效应相似。因此,与单克隆抗体AA4结合的表面神经节苷脂可能在调节分泌事件中发挥作用。