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肥大细胞克隆:细胞成熟分析模型

Mast cell clones: a model for the analysis of cellular maturation.

作者信息

Galli S J, Dvorak A M, Marcum J A, Ishizaka T, Nabel G, Der Simonian H, Pyne K, Goldin J M, Rosenberg R D, Cantor H, Dvorak H F

出版信息

J Cell Biol. 1982 Nov;95(2 Pt 1):435-44. doi: 10.1083/jcb.95.2.435.

Abstract

Cloned mouse mast cells resemble, by ultrastructure, immature mast cells observed in vivo. These mast cell clones can be grown in the absence of any other cells, facilitating direct investigations of their biochemistry and function. We find that cloned mast cells express plasma membrane receptors (Fc epsilon R) that bind mouse IgE with an equilibrium constant (KA) similar to that of normal mouse peritoneal mast cells. In addition, cloned mast cells do not display detectable la antigens and cannot enhance lg secretion when added to lymphocyte cultures or mediate natural killer lysis. In the presence of 1 mM sodium butyrate, cloned mast cells stop dividing and acquire abundant electron-dense cytoplasmic granules similar to those of mature mast cells. Their histamine content increases concomitant with cytoplasmic granule maturation and may exceed that of untreated mast cells by 50-fold. Unlike peritoneal mast cells, cloned mast cells incorporate 35SO4 into chondroitin sulfates rather than heparin. These findings demonstrate that, unlike fully differentiated mouse peritoneal mast cells, cloned immature mouse mast cells contain no heparin and low levels of histamine. In addition, they establish that high-affinity Fc epsilon R are expressed early in mast cell maturation, well before completion of cytoplasmic granule synthesis and mediator storage.

摘要

克隆的小鼠肥大细胞在超微结构上类似于体内观察到的未成熟肥大细胞。这些肥大细胞克隆可以在没有任何其他细胞的情况下生长,便于直接研究它们的生物化学和功能。我们发现克隆的肥大细胞表达质膜受体(FcεR),该受体以与正常小鼠腹膜肥大细胞相似的平衡常数(KA)结合小鼠IgE。此外,克隆的肥大细胞不显示可检测到的Ia抗原,当添加到淋巴细胞培养物中时不能增强Ig分泌,也不能介导自然杀伤细胞裂解。在1 mM丁酸钠存在下,克隆的肥大细胞停止分裂并获得与成熟肥大细胞相似的大量电子致密细胞质颗粒。它们的组胺含量随着细胞质颗粒成熟而增加,可能比未处理的肥大细胞高出50倍。与腹膜肥大细胞不同,克隆的肥大细胞将35SO4掺入硫酸软骨素而不是肝素中。这些发现表明,与完全分化的小鼠腹膜肥大细胞不同,克隆的未成熟小鼠肥大细胞不含肝素且组胺水平较低。此外,它们证实高亲和力FcεR在肥大细胞成熟早期表达,远在细胞质颗粒合成和介质储存完成之前。

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