Expression and function of the interleukin 7 receptor in murine lymphocytes.

T Sudo(Toray Industries, Inc. (Japan)), Satoru Nishikawa(Toray Industries, Inc. (Japan)), Noriko Ohno(Toray Industries, Inc. (Japan)), Naoko Akiyama(Toray Industries, Inc. (Japan)), Masatada Tamakoshi(Toray Industries, Inc. (Japan)), Hisahiro Yoshida(Toray Industries, Inc. (Japan)), Satoru Nishikawa(Toray Industries, Inc. (Japan))
Proceedings of the National Academy of Sciences
October 1, 1993
Cited by 484Open Access

Abstract

A monoclonal antibody, A7R34, that recognizes the high-affinity interleukin 7 receptor (IL-7Ra) and blocks the binding between IL-7 and IL-7Ra has been produced. Cell surface staining with A7R34 demonstrated that IL-7Ra is expressed in both B- and T-cell lineages. In the bone marrow, immature B-lineage cells that do not express surface IgM were IL-7Ra+. In the thymus, IL-7Ra was detected in CD4-8- T cells and also in CD4 or CD8 single-positive cells but not in CD4+8+ double-positive cells. In the peripheral lymphoid tissues, both CD4 and CD8 single-positive cells were the major cell types that express IL-7Ra. Addition of A7R34 to a long-term B-precursor-cell culture inhibited proliferation of the B-lineage cells, indicating that IL-7 is an absolute requirement for in vitro B-cell genesis. Consistent with this in vitro result, continuous injection of A7R34 into an adult mouse resulted in a decrease of B-precursor cells and also of thymocytes, whereas a considerable fraction of mature B and T cells in the peripheral tissues persisted over 2 weeks of the experiment. When A7R34 injection is started from day 14 of gestation, it is possible to produce mice that lack B cells. These results indicate that IL-7 is an essential molecule for generation of both B and T cells in murine bone marrow and thymus, respectively. Moreover, IL-7Ra would be the sole receptor system regulating these processes.


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