Mono- and bi-allelic expression of insulin-like growth factor II gene in human muscle tumors |
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Authors: | Pedone, Paolo V. Tirabosco, Roberto Cavazzana, Andrea O. Ungaro, Paola Basso, Giuseppe Luksch, Roberto Carli, Modesto Bruni, Carmelo B. Frunzio, Rodolfo Riccio, Andrea |
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Affiliation: | Centro di Endocrinologia ed Oncologia Spenmentale, CNR, Dipartimento di Biologia e Pataologia Cellulare e Molecolare Torvergata, Italy 1Istituto di Anatomia Patologica, Università di Roma Torvergata, Italy 2II Clinica Pediatrica, Università di Padova FONOP, Milano, Italy 3Gruppo Biologico Oncologia Tumori Solidi Pediatrici FONOP, Milano, Italy 4Istituto Nazionale dei Tumori Milano, Italy 5Dipartimento di Chimica Organica e Biologica, Università di Napoli Federico II Torvergata, Italy |
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Abstract: | Insulin-like growth factor II (IGF-II) is a mitogen for manycell types and an important modulator of muscle growth and differentiation.IGF-II gene is prevalently expressed during prenatal developmentand its gene activity is regulated by genomic imprinting, inthat the allele inherited from the father is active and theallele inherited from the mother is inactive in most normaltissues. IGF-II expression is activated in several types ofhuman neoplasms and an alteration of IGF-II imprinting has beendescribed in BeckwithWiedemann syndrome and Wilms' tumour.Here we show that monoallelic expression of IGF-II gene is conservedin normal adult muscle tissue whereas two or more copies ofactive IGF-II alleles, arising by either relaxation of imprintingor duplication of the active allele, are found in 9 out of 11(82%) rhabdomyo-sarcomas retaining heterozygosity at 11p15,regardless of the histological subtype. Since IGF-II has beenindicated as an autocrine growth factor for rhabdomyosarcomacells, these findings strongly suggest that acquisition of adouble dosage of active IGF-II gene is an important step forthe initiation or progression of rhabdomyosarcoma tumorigenesis.Among different types of muscle tumors, relaxation of imprintingseems to arise prevalently in rhabdomyosarcomas, since we havedetected only one case of partial reactivation of the maternalIGF-II allele out of 7 lelomyosarcomas tested. |
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