Fibroblast-Secreted Macrophage Colony-Stimulating Factor Is Responsible for Generation of Biphenotypic B/Macrophage Cells from a Subset of Mouse B Lymphocytes

Author:

Borrello Melinda A.123,Phipps Richard P.1245

Affiliation:

1. *Cancer Center and Departments of

2. †Microbiology and Immunology,

3. ¶Eastman Dental Center, Rochester, NY 14620

4. ‡Pediatrics, and

5. §Environmental Medicine, University of Rochester School of Medicine and Dentistry, Rochester, NY 14642; and

Abstract

Abstract Normal and malignant CD5+ B lymphocytes can develop macrophage-like characteristics. One stimulus of this phenotypic shift is culture of normal mouse splenic B lymphocytes with splenic fibroblasts or their conditioned media. These biphenotypic B/macrophage (B/Mφ) cells simultaneously display macrophage characteristics, such as phagocytosis and F4/80 expression, while retaining B cell features, including expression of surface Ig, CD5, B220, and rearranged Ig genes. The present study investigated the fibroblast-secreted factor that promotes this phenotypic change from B cell to B/Mφ cell. RT-PCR analysis demonstrated that mRNA for M-CSF is produced by splenic fibroblasts. Recombinant M-CSF (CSF-1) could replace fibroblast-conditioned medium to elicit the development and survival of B/Mφ cells from splenic B lymphocytes. In addition, neutralization of fibroblast-secreted M-CSF with specific mAbs abrogated the ability of conditioned supernatants to promote outgrowth of B/Mφ cells. The transition from B lymphocyte to B/Mφ cell was marked by the kinetic appearance of mRNA for the M-CSF receptor, c-fms, at day 3 following culture initiation. These results demonstrate that M-CSF is important in the development and physiology of mouse B/Mφ cells and potentially in the growth of human biphenotypic hematological malignancies. Interestingly, the presence of IFN-γ in splenic B lymphocyte cultures abrogated the effect of fibroblast-conditioned medium or M-CSF on outgrowth of B/Mφ cells. Furthermore, these findings suggest that a Th1 microenvironment favored by typical macrophages is detrimental to the outgrowth of B/Mφ cells.

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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