Bone Marrow-Infiltrating Human Neuroblastoma Cells Express High Levels of Calprotectin and HLA-G Proteins
Morandi, Fabio; Scaruffi, Paola; Gallo, Fabio; Stigliani, Sara; Moretti, Stefano; Bonassi, Stefano; Gambini, Claudio; Mazzocco, Katia; Fardin, Paolo; Haupt, Riccardo; Pistoia, Vito; Tonini, Gian Paolo; Corrias, Maria Valeria (2012), Bone Marrow-Infiltrating Human Neuroblastoma Cells Express High Levels of Calprotectin and HLA-G Proteins, PLoS ONE, 7, 1, p. 11. 10.1371/journal.pone.0029922
Type
Article accepté pour publication ou publiéDate
2012Journal name
PLoS ONEVolume
7Number
1Publisher
Public Library of Science
Pages
11
Publication identifier
Metadata
Show full item recordAuthor(s)
Morandi, FabioGaslini Institute
Scaruffi, Paola
National Cancer Research Institute
Gallo, Fabio
National Cancer Research Institute
Stigliani, Sara
National Cancer Research Institute
Moretti, Stefano

Laboratoire d'analyse et modélisation de systèmes pour l'aide à la décision [LAMSADE]
Bonassi, Stefano
San Raffaele Pisana IRCCS
Gambini, Claudio
Gaslini Institute
Mazzocco, Katia
National Cancer Research Institute
Fardin, Paolo
Gaslini Institute
Haupt, Riccardo
Gaslini Institute
Pistoia, Vito
Gaslini Institute
Tonini, Gian Paolo
National Cancer Research Institute
Corrias, Maria Valeria
Gaslini Institute
Abstract (EN)
Metastases in the bone marrow (BM) are grim prognostic factors in patients with neuroblastoma (NB). In spite of extensive analysis of primary tumor cells from high- and low-risk NB patients, a characterization of freshly isolated BM-infiltrating metastatic NB cells is still lacking. Our aim was to identify proteins specifically expressed by metastatic NB cells, that may be relevant for prognostic and therapeutic purposes. Sixty-six Italian children over 18 months of age, diagnosed with stage 4 NB, were included in the study. Metastatic NB cells were freshly isolated from patients' BM by positive immunomagnetic bead manipulation using anti-GD2 monoclonal antibody. Gene expression profiles were compared with those obtained from archived NB primary tumors from patients with 5y-follow-up. After validation by RT-qPCR, expression/secretion of the proteins encoded by the up-regulated genes in the BM-infiltrating NB cells was evaluated by flow cytometry and ELISA. Compared to primary tumor cells, BM-infiltrating NB cells down-modulated the expression of CX3CL1, AGT, ATP1A2 mRNAs, whereas they up-regulated several genes commonly expressed by various lineages of BM resident cells. BM-infiltrating NB cells expressed indeed the proteins encoded by the top-ranked genes, S100A8 and A9 (calprotectin), CD177 and CD3, and secreted the CXCL7 chemokine. BM-infiltrating NB cells also expressed CD271 and HLA-G. We have identified proteins specifically expressed by BM-infiltrating NB cells. Among them, calprotectin, a potent inflammatory protein, and HLA-G, endowed with tolerogenic properties facilitating tumor escape from host immune response, may represent novel biomarkers and/or targets for therapeutic intervention in high-risk NB patients.Subjects / Keywords
bone marrow; Neuroblastoma; gene expressionRelated items
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