Retroviral expression of the human IL-2 gene in a murine T cell line results in cell growth autonomy and tumorigenicity. |
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Authors: | G Yamada Y Kitamura H Sonoda H Harada S Taki R C Mulligan H Osawa T Diamantstein S Yokoyama T Taniguchi |
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Affiliation: | Institute for Molecular and Cellular Biology, Osaka University, Japan. |
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Abstract: | In mature T lymphocytes (T cells) the regulated expression of the genes for interleukin-2 (IL-2) and its receptor (IL-2R) constitutes an essential part in controlling the cell growth. Evidence has been provided which suggests the involvement of an aberrant function of the IL-2 system in developing T cell neoplasms, particularly the adult T cell leukemia/lymphoma (ATL). As an approach to examine the extent of the IL-2 system contribution to T cell neoplasms, we created the experimental conditions wherein both IL-2 and IL-2R are expressed constitutively in a murine T cell line. We made use of a retroviral vector to infect an IL-2-dependent CTLL-2 line and lead to the expression of human IL-2. Here, we show that the virus-infected cells not only proliferate in vitro in the absence of exogenously supplied IL-2 under certain conditions, but also develop tumors (lymphomas) in nude and syngeneic mice. |
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