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小鼠腹腔巨噬细胞内源性过氧化物酶活性驻留模式的发展与分化抗原F4/80的表达相一致。一种免疫过氧化物酶标记和内源性过氧化物酶细胞化学的联合方法。

The development of the resident pattern of endogenous peroxidatic activity in mouse peritoneal macrophages coincides with the expression of the differentiation antigen F4/80. A combined method for immunoperoxidase labeling and endogenous peroxidase cytochemistry.

作者信息

Hoefsmit E C, Schadee-Eestermans I L, Beelen R H

出版信息

J Histochem Cytochem. 1986 May;34(5):633-40. doi: 10.1177/34.5.3517147.

Abstract

In the mouse the maturation of mononuclear phagocytes was followed by comparing the ultrastructural pattern of endogenous peroxidatic activity (PA) at different time points during an acute peritonitis induced with newborn calf serum (NCS). Exudate macrophages demonstrate PA only in lysosomes, whereas resident macrophages have reaction product in the nuclear envelope (NE) and rough endoplasmic reticulum (RER). Transitional cells called "exudate-resident" macrophages have PA in the NE, RER, and some virginal lysosomes. In addition, peroxidase-negative macrophages were also present. A monoclonal antibody, F4/80, that specifically recognizes a mouse macrophage differentiation antigen (Austyn and Gordon, 1981) was used in this study. To compare the indirect immunoperoxidase labeling of this antigen and the endogenous peroxidase cytochemistry on the cellular level, a combined method was developed. Finally, the method was applied to the peritoneal cells at different time points after intraperitoneal injection of NCS in mice. The relative numbers of cells demonstrating the different patterns of endogenous PA and the proportions of each subpopulation expressing F4/80 antigen were estimated. It appeared that the expression of the antigen F4/80 coincides with the development of the resident pattern of PA. It is therefore concluded that the macrophages with the resident pattern of endogenous peroxidase are derived from monocyte-like exudate macrophages. In addition, the results indicate that both exudate-resident macrophages and at least a part of the peroxidase-negative macrophages are transitional forms.

摘要

通过比较新生小牛血清(NCS)诱导的急性腹膜炎不同时间点内源性过氧化物酶活性(PA)的超微结构模式,研究了小鼠单核吞噬细胞的成熟过程。渗出液巨噬细胞仅在溶酶体中显示PA,而驻留巨噬细胞在核膜(NE)和粗面内质网(RER)中有反应产物。称为“渗出液 - 驻留”巨噬细胞的过渡细胞在NE、RER和一些原始溶酶体中有PA。此外,还存在过氧化物酶阴性巨噬细胞。本研究使用了一种特异性识别小鼠巨噬细胞分化抗原的单克隆抗体F4/80(Austyn和Gordon,1981)。为了在细胞水平上比较该抗原的间接免疫过氧化物酶标记和内源性过氧化物酶细胞化学,开发了一种联合方法。最后,将该方法应用于小鼠腹腔注射NCS后不同时间点的腹腔细胞。估计了显示内源性PA不同模式的细胞的相对数量以及表达F4/80抗原的每个亚群的比例。结果表明,抗原F4/80的表达与PA驻留模式的发展一致。因此得出结论,具有内源性过氧化物酶驻留模式的巨噬细胞来源于单核细胞样渗出液巨噬细胞。此外,结果表明渗出液 - 驻留巨噬细胞和至少一部分过氧化物酶阴性巨噬细胞都是过渡形式。

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