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CURRICULUM VITAE Nome: Luigi Varesio Data e Luogo di nascita: 6 Luglio 1951; Torino, Italia Cittadinanza: USA, Italiana Stato civile: Sposato; due figli Posizione Attuale: Direttore del Laboratorio di Biologia Molecolare, Istituto Giannina Gaslini Titoli di Studio: 1970 - Maturità Scientifica Liceo "G.Ferraris", Torino 1974 - Laurea in Scienze Biologiche (con lode) presso l’Università' di Torino 1977 - Specializzazione in Microbiologia presso l' Università di Torino 2014 Corso di formazione manageriale per Dirigenti di Struttura Complessa presso Cisef, Genova Breve elenco degli impieghi: 1969-1970 - Studente interno presso i Laboratori del Liceo Scientifico “G. Ferraris” di Torino 1970-1974 - Studente interno presso l’Istituto di Microbiologia dell'Universita' di Torino. 1974-1977 - Borsa di studio Postdottorato presso il Dipartimento di Microbiologia, Scuola di Medicina, Universita' di Torino. 1977-1980 - Visiting Fellow, Laboratory Immunodiagnosis National Cancer Institute, Bethesda, MD, USA 1980-1981 - Visiting Associate, Laboratory Immunodiagnosis National Cancer Institute, Bethesda, MD, USA 1981-1983 - Visiting Associate, Biological Response Modifiers Program, National Cancer Institute, Frederick, MD, USA 1983-1993 - Visiting Scientist, Laboratory Molecular Immunoregulation, Biological Response Modifiers Program, National Cancer Institute, Frederick, MD, USA 1983-1985 - Direttore, Sezione di Immunobiologia, Laboratory of Molecular Immunoregulation, National Cancer Institute, Frederick, MD, USA 1985-1993 - Direttore, Sezione di Immunobiologia, Laboratory Experimental Immunology, National Cancer Institute, Frederick, MD, USA 1993-1996- Direttore, sezione Macrophage Cell Biology, Laboratory Experimental Immunology, National Cancer Institute, Frederick, MD, USA 1995-1998 - Direttore, Servizio di Genetica Molecolare, Istituto “G. Gaslini”, Genova, Italia 1994-oggi - Direttore, Servizio di Biologia Molecolare, Istituto “G. Gaslini”, Genova, Italia 1999-oggi - Professore, Biologia Molecolare, Scuola di Specializzazione in Malattie Infettive, Facoltà di Medicina, Università di Genova, Genova, Italia 1999-oggi - Professore di Biologia Molecolare presso la Scuola di Specializzazione in Genetica Medica, Facoltà di Medicina, Genova, Italia 1 Pubblicazioni ultimi 5 anni: 1. Varesio L, Battaglia F, Raggi F, Ledda B, Bosco MC. Macrophage-inflammatory protein-3alpha/CCL-20 is transcriptionally induced by the iron chelator desferrioxamine in human mononuclear phagocytes through nuclear factor (NF)-kappaB. Mol Immunol 2010;47:685-693. 2. Fardin P, Barla A, Mosci S et al. A biology-driven approach identifies the hypoxia gene signature as a predictor of the outcome of neuroblastoma patients. Mol Cancer 2010;9:185. 3. Fardin P, Cornero A, Barla A et al. Identification of multiple hypoxia signatures in neuroblastoma cell lines by l1-l2 regularization and data reduction. J Biomed.Biotechnol. 2010;2010:878709. 4. Bosco MC, Varesio L. Monocytic cell gene regulation by the hypoxic synovial environment in juvenile idiopathic arthritis: implications for disease pathogenesis. Journal of Clinical Rheumatology & Musculoskeletal Medicine 2010;1:1-9. 5. Bosco MC, Pierobon D, Blengio F et al. Hypoxia modulates the gene expression profile of immunoregulatory receptors in human mature dendritic cells: identification of TREM-1 as a novel hypoxic marker in vitro and in vivo. Blood 2011;117:2625-2639. 6. Sica A, Melillo G, Varesio L. Hypoxia: a double-edged sword of immunity. J Mol Med 2011;89:657-665. 7. Ognibene M, Barbieri O, Vanni C et al. High frequency of development of B cell lymphoproliferation and diffuse large B cell lymphoma in Dbl knock-in mice. J Mol Med 2011;89:493-504. 8. Resaz R, Emionite L, Vanni C et al. Treatment of newborn G6pc(-/-) mice with bone marrow-derived myelomonocytes induces liver repair. J Hepatol. 2011;55:1263-1271. 9. Ognibene M, Vanni C, Segalerba D et al. The tumor suppressor hamartin enhances Dbl transforming activity through interaction with ezrin. J Biol Chem. 2011;89:493-504. 10. Blengio F, Raggi F, Pierobon D et al. The hypoxic environment reprograms the cytokine/chemokine expression profile of human mature dendritic cells. Immunobiology 2013;218:76-89. 11. Cornero A, Acquaviva M, Fardin P et al. Design of a multi-signature ensemble classifier predicting neuroblastoma patients' outcome. BMC Bioinformatics 2012;13 Suppl 4:S13. 12. Petecchia L, Sabatini F, Usai C et al. Cytokines induce tight junction disassembly in airway cells via an EGFR-dependent MAPK/ERK1/2-pathway. Lab Invest 2012;92:1140-1148. 2 13. Bosco MC, Varesio L. Dendritic cell reprogramming by the hypoxic environment. Immunobiology 2012;217:1241-1249. 14. Cattelani S, Ferrari-Amorotti G, Galavotti S et al. The p53 codon 72 Pro/Pro genotype identifies poor-prognosis neuroblastoma patients: correlation with reduced apoptosis and enhanced senescence by the p53-72P isoform. Neoplasia. 2012;14:634-643. 15. Molenaar JJ, Domingo-Fernandez R, Ebus ME et al. LIN28B induces neuroblastoma and enhances MYCN levels via let-7 suppression. Nat Genet. 2012;44:1199-1206. 16. Pierobon D, Bosco MC, Blengio F et al. Chronic hypoxia reprograms human immature dendritic cells by inducing a proinflammatory phenotype and TREM-1 expression. Eur.J Immunol 2013;43:949-966. 17. Cangelosi D, Blengio F, Versteeg R et al. Logic Learning Machine creates explicit and stable rules stratifying neuroblastoma patients. BMC Bioinformatics 2013;14:S12. 18. Amendola R, Cervelli M, Tempera G et al. Spermine metabolism and radiation-derived reactive oxygen species for future therapeutic implications in cancer: an additive or adaptive response. Amino.Acids 2013;13:1579-1599. 19. Bosco MC, Varesio L. Hypoxia and Gene Expression. In: Melillo G, ed. Hypoxia and cancer.: Humana Press; 2013:91-119. 20. Balsamo M, Manzini C, Pietra G et al. Hypoxia downregulates the expression of activating receptors involved in NK-cell-mediated target cell killing without affecting ADCC. Eur.J.Immunol. 2013;43:2756-2764. 21. Ognibene M, Vanni C, Blengio F et al. Identification of a novel mouse Dbl protooncogene splice variant: Evidence that SEC14 domain is involved in GEF activity regulation. Gene 2014;537:220-229. 3