Insulin-like growth factors are involved in the paracrine growth regulation of human breast tumor cells. IGF2 is imprinted in most tissues, and shows expression of the paternal allele only. To investigate whether disruption of this monoallelic IGF2 expression is involved in breast cancer development, a series of primary tumors and adjacent, histologically normal, breast tissue samples, as well as matched primary in vitro fibroblast cultures were studied. Biallelic expression (partial) of IGF2 was found in the majority of in vivo samples, and corresponding fibroblast cultures, while monoallelic expression was found in a normal breast sample. In contrast, H19, a closely apposed, but reciprocally imprinted gene, assumed to be regulated by a common control element, showed retention of monoallelic H19 expression in all in vivo and in the majority of in vitro samples. These data indicate that IGF2, but not H19, is prone to loss of imprinting in breast cancer. Copyright (C) 1998 Federation of European Biochemical Societies.

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Keywords Breast cancer, Genomic imprinting, Insulin-like growth factor, Stromal fibroblast
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Journal F E B S Letters
van Roozendaal, C.E, Gillis, A.J.M, Klijn, J.G.M, van Ooijen, B, Claassen, C.J, Eggermont, A.M.M, … Looijenga, L.H.J. (1998). Loss of imprinting of IGF2 and not H19 in breast cancer, adjacent normal tissue and derived fibroblast cultures. F E B S Letters, 437(1-2), 107–111. doi:10.1016/S0014-5793(98)01211-3