Alterations in gene expression associated with stepwise acquisition of malignancy in murine cytotoxic T cell lines

doi:10.1093/intimm/5.9.1075

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International Immunology, Vol. 5, No. 9, pp. 1075-1083,September 1993
© 1993 Japanese Society for Immunology

Alterations in gene expression associated with stepwise acquisition of malignancy in murine cytotoxic T cell lines

A. Ehrfeld, A. Zgaga-Griesz, A. Würch, A. Potocnic, C. Kastenholz, M. M. Simon and K. Eichmann

Max-Planck-lnstitut fur Immunbiologie 79108 Freiburg, Germany

Correspondence to: Correspondence to: A. Ehrfeld

We have isolated a series of variant cell lines from a murineCD8⁺ T cell clone representing distinct stages in stepwise acquisitionof malignancy. A first type of variant has acquired independencyof restimulation with MHC/Ag but has kept dependence on IL-2for continuous growth in culture. A second type of variant hasacquired, in addition, independency of IL-2. A third type ofvariant was isolated from tumors induced upon injection of IL-2independent variants into syngenelc mice. Clonal relatednessbetween the cell lines was ascertained by Southern blot andsequence analyses of their TCRß chain genes. The celllines were analyzed for their expression of genes typical forCD8⁺ T cells, using Northern blot hybridization, flow cytometry,and functional methods. Concentrating on the transition fromIL-2 dependent to IL-2 independent cellular growth, we findthe same triad of changes in two independently derived groupsof variant cell lines: loss of expression of the CD8 ${alpha}$ gene withconcomitant loss of CD8 from the cell surface, a slight butsignificant overexpresslon of IL-2R ${alpha}$ and ß chains withincreased low affinity IL-2 binding sites, and constitutiveoverexpresslon of c-myc. Autocrine IL-2 dependent growth couldbe excluded. Expression of p56^lck did not vary between the celllines. We discuss the possibility that IL-2 independent growthmay be associated with intracellular redistribution of p56^lckfrom CD8 ${alpha}$ to IL-2Rß, thus generating constitutlvelyactive IL-2R. Ex vivo estabilshed tumor variants differed fromtheir parental culture cell lines by their constitutive secretionof IFN-. Since tumor variants derived from different organsof several individual mice showed this phenotype, we suggestthat constitutive IFN- secretion may be causally related toin vivo tumor formation, for example by induction of endothelialadhesion molecules facilitating tumor cell extravasation. Anumber of functional molecules did not significantly vary betweencell lines, including components of ${alpha}$ ß CD3 TCR, CD45,LFA-1, and MHC class I.

Keywords: CD8, c-myc, gene expression, IFN- ${gamma}$ , IL-2 receptor, T cell activation, T cell malignancy

Received 30 November 1992, accepted 21 May 1993.

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