Murine macrophage precursor characterization. II. Monoclonal antibodies against macrophage precursor antigens
- 1 January 1990
- journal article
- research article
- Published by Wiley in European Journal of Immunology
- Vol. 20 (1) , 27-34
- https://doi.org/10.1002/eji.1830200105
Abstract
The aim of the present study was the phenotypical analysis of early stages in macrophage (Mϕ) differentiation. For this purpose, we produced a panel of syngeneic rat hybridomas, which secreted antibodies (mAb) against Mϕ precursor antigens. As immunogens we used immortalized Mϕ precursors (P. J. M. Leenen et al., Eur. J. Immunol. 1990. 20: 15). We screened the obtained mAb in the following in vitro models of Mϕ differentiation: (a) a panel of Mϕ cell lines ordered in a linear differentiated sequence; (b) immature and mature mononuclear phagocytes obtained from bone marrow (BM) culture; (c) a panel of Mϕ precursor hybrids, and (d) differentiated and control Mϕ precursor hybrid cells. Four mAb, ER‐MP12, ER‐MP20, ER‐MP54 and ER‐MP58, were selected. These mAb recognize antigens which disappear in the course of Mϕ differentiation. Next, we investigated whether these mAb also recognized Mϕ precursors in normal BM. For this purpose, ER‐MP‐positive and ‐negative BM fractions were isolated using a fluorescence‐activated cell sorter. Fractions were cultured in Mϕ‐colony‐stimulating factor‐containing conditioned medium, and the resulting mature Mϕ progeny was quantified using the MTT assay. The present experiments indicate that ER‐MP12 and ER‐MP20 detect a subpopulation of BM Mϕ precursors, whereas ER‐MP58 stains virtually all Mϕ precursors. Biochemical analysis of radioiodinated antigens revealed that these mAb recognize different molecules. ER‐MP12 and ER‐MP20 bound to single‐chain (glyco)proteins of 140 kDa and 14 kDa, respectively. ER‐MP54 precipitated multiple polypeptides, of which the major chains have an apparent molecular mass of 90, 80‐85 and 70‐75 kDa. Based on the molecular mass of the recognized antigens and the mAb specificities we conclude that ER‐MP12, ER‐MP54 and ER‐MP58 recognize hitherto unknown antigens of murine Mϕ precursor cells. The antigen detected by ER‐MP20 is most likely identical to Ly‐6C.This publication has 39 references indexed in Scilit:
- Murine macrophage precursor characterization. I. Production, phenotype and differentiation of macrophage precursor hybridsEuropean Journal of Immunology, 1990
- Monocytes and MacrophagesNew England Journal of Medicine, 1988
- Macrophages in T and B Cell Compartments and Other Tissue Macrophages Recognized by Monoclonal Antibody MOMA‐2Scandinavian Journal of Immunology, 1987
- Single-cell immuno-β-galactosidase staining of heterogeneous populations. Practical application on limited cell numbersJournal of Molecular Histology, 1987
- There is more than one interleukin 1Immunology Today, 1986
- Synergism between hemopoietic growth factors (HGFs) detected by their effects on cells bearing receptors for a lineage specific HGF: Assay of hemopoietin‐1Journal of Cellular Physiology, 1985
- DMSO-induced terminal differentiation and trisomy 15 in myeloid cell line transformed by the Rauscher murine leukemia virusCell Differentiation, 1981
- F4/80, a monoclonal antibody directed specifically against the mouse macrophageEuropean Journal of Immunology, 1981
- Functional macrophage cell lines transformed by abelson leukemia virusCell, 1978
- Lymphosarcoma cell growth is selectively inhibited by B lymphocyte mitogens: LPS, dextran sulfate and PPDBiochemical and Biophysical Research Communications, 1974