In vitro growth of murine T cells. IV. Use of T-cell growth factor to clone lymphoid cells |
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Authors: | S A Rosenberg P J Spiess S Schwarz |
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Affiliation: | Departments of Microbiology, Pathology, and Medicine and the Cancer Research Center, Boston University School of Medicine, Boston, Massachusetts 02118 USA |
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Abstract: | Murine bone marrow cells can suppress the in vitro primary antibody response of normal spleen cells without apparent cytotoxicity. The bone marrow cells suppress the response to both T-dependent (SRBC) and T-independent (DNP-Ficoll) antigens. When bone marrow cells are fractionated on a sucrose density gradient, the suppressive activity is found in the residue rather than the lymphocyte fraction. The suppressive activity is either unaffected or enhanced by treatment with anti-T- and anti-B-cell serums. Pretreatment of mice with phenylhydrazine which reduces the number of pre-B cells did not reduce the suppressive activity of their bone marrow cells. Suppressive activity is abolished by irradiation of the marrow cells in vitro with 1000 R prior to assay. The activity is present in the marrow of thymus deficient (nude) mice, infant mice, and mice which have been made polycythemic by transfusion. Furthermore, the suppressor cell can phagocytize iron carbonyl particles, is slightly adherent to plastic and Sephadex G-10, and can bind to EA monolayers. We conclude that the suppressor cell is not a mature lymphocyte or granulocyte nor a member of the erythrocytic series, but is likely to be an immature cell possibly of the myeloid series. We speculate on the physiologic role of this cell. |
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Keywords: | Address reprint requests to Steven A. Rosenberg M.D. Ph.D. Chief of Surgery National Cancer Institute Building 10 Room 10N116 Bethesda Md. 20205. |
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