巨噬细胞对正在经历程序性细胞死亡(凋亡)的细胞的识别。
Macrophage recognition of cells undergoing programmed cell death (apoptosis).
作者信息
Duvall E, Wyllie A H, Morris R G
出版信息
Immunology. 1985 Oct;56(2):351-8.
Abstract
As a model for the recognition of effete cells by their viable neighbours. BALB/c mouse thymocytes were coincubated with isologous peritoneal macrophages. The macrophages bound preferentially to thymocytes undergoing apoptosis, a mode of death induced in these cells by treatment with the glucocorticoid hormone methyl-prednisolone. Binding occurred in the absence of serum and was inhibited by N,N'-diacetyl chitobiose, N-acetyl glucosamine and, to a lesser extent, by N-acetyl galactosamine and D-galactose. L-fucose, D-mannose and N-acetyl neuraminic acid had no effect. The results suggest the presence of lectin-like molecules on the surface of the macrophage that recognize changes in the cell-surface carbohydrate of the apoptotic cell. The pattern of inhibition of binding by monosaccharides differs from that of previously described endogenous mammalian lectins.
摘要
作为活细胞识别衰老细胞的模型,将BALB/c小鼠胸腺细胞与同源腹腔巨噬细胞共同孵育。巨噬细胞优先结合正在经历凋亡的胸腺细胞,凋亡是这些细胞经糖皮质激素甲泼尼龙处理后诱导的一种死亡方式。结合在无血清条件下发生,并被N,N'-二乙酰壳二糖、N-乙酰葡糖胺抑制,在较小程度上被N-乙酰半乳糖胺和D-半乳糖抑制。L-岩藻糖、D-甘露糖和N-乙酰神经氨酸没有作用。结果表明巨噬细胞表面存在凝集素样分子,可识别凋亡细胞表面碳水化合物的变化。单糖对结合的抑制模式与先前描述的内源性哺乳动物凝集素不同。
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