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Neuroblastoma specific effects of DR-nm23 and its mutant forms on differentiation and apoptosis

TitleNeuroblastoma specific effects of DR-nm23 and its mutant forms on differentiation and apoptosis
Publication TypeArticolo su Rivista peer-reviewed
Year of Publication2000
AuthorsNegroni, Anna, Venturelli D., Tanno Barbara, Amendola R., Ransac S., Cesi Vincenzo, Calabretta B., and Raschellà G.
JournalCell Death and Differentiation
Volume7
Pagination843-850
ISSN13509047
Keywordsanimal cell, Apoptosis, article, biochemistry, Catalysis, cell fractionation, cell structure, controlled study, cytoplasm, enzyme activity, Gene expression, gene location, gene overexpression, hematopoietic cell, Immunoprecipitation, metastasis, mitochondrion, mouse, Multigene Family, mutant, nerve cell differentiation, Neuroblastoma, neuroblastoma cell, nonhuman, nucleoside diphosphate kinase, Phosphorylation, polymer, priority journal, protein binding, protein protein interaction, serine, serum, tissue specificity, tumor suppressor gene
Abstract

DR-nm23 belongs to a gene family which includes nm23-H1, originally identified as a candidate metastasis suppressor gene. Nm23 genes are expressed in different tumor types where their levels have been alternatively associated with reduced or increased metastatic potential. Nm23-H1, -H2, DRnm23 and nm23-H4 all possess NDP kinase activity. Overexpression of DR-nm23 inhibits differentiation and promotes apoptosis in hematopoietic cells. By contrast, it induces morphological and biochemical changes associated with neural differentiation in neuroblastoma cells. In this study, we show that mutations in the catalytic domain and in the serine 61 phosphorylation site, possibly required for protein-protein interactions, impair the ability of DR-nm23 to induce neural differentiation. Moreover, neuroblastoma cells overexpressing wild-type or mutant DR-nm23 are less sensitive to apoptosis triggered by serum withdrawal. By subcellular fractionation, wild-type and mutant DR-nm23 localize in the cytoplasm and prevalently in the mitochondrial fraction. In coimmunoprecipitation experiments, wild-type DR-nm23 binds other members of nm23 family, but mutations in the catalytic and in the RGD domains and in serine 61 inhibit the formation of hetero-multimers. Thus, the integrity of the NDP kinase activity and the presence of a serine residue in position 61 seem essential for the ability of DR-nm23 to trigger differentiation and to bind other Nm23 proteins, but not for the anti-apoptotic effect in neuroblastoma cells. These studies underline the tissue specificity of the biological effects induced by DR-nm23 expression.

Notes

cited By 40

URLhttps://www.scopus.com/inward/record.uri?eid=2-s2.0-0033828759&doi=10.1038%2fsj.cdd.4400720&partnerID=40&md5=18a52c91d2ee8093d4f2dc8437137e32
DOI10.1038/sj.cdd.4400720
Citation KeyNegroni2000843