Adult cardiac progenitor cells (CPCs), isolated as cardiosphere-derived cells (CDCs), represent promising candidates for cardiac regenerative therapy. CDCs can be expanded in vitro manyfolds without losing their differentiation potential, reaching numbers that are appropriate for clinical applications. Since mechanisms of successful CDC survival and engraftment in the damaged myocardium are still critical and unresolved issues, we aimed at deciphering possible key factors capable of bolstering CDC function. In particular, the response and the phenotype of CDCs exposed to low concentrations of the multifunctional cytokine tumor necrosis factor a (TNF-alpha), known to be capable of activating cell survival pathways, have been investigated. Furthermore, differential biological responses of CDCs from male and female donors, in terms of cell cycle progression and cell spreading, have also been assessed. The results obtained indicate that (i) the intracellular signaling activated in our experimental conditions is most likely due to the prosurvival and proliferative signaling of TNF-alpha receptor 2 and that (ii) cells from female patients appear more responsive to TNF-alpha treatment in terms of cell cycle progression and migration ability. In conclusion, the present report highlights the hypothesis that TNF-stimulated CDCs isolated from females may represent a promising candidate for cardiac regenerative therapy applications.

Sex differences of human cardiac progenitor cells in the biological response to TNF-α treatment / Straface, Elisabetta; Gambardella, Lucrezia; Pagano, Francesca; Angelini, Francesco; Ascione, Barbara; Vona, Rosa; De Falco, Elena; Cavarretta, Elena; La Russa, Raffaele; Malorni, Walter; Frati, Giacomo; Chimenti, Isotta.. - In: STEM CELLS INTERNATIONAL. - ISSN 1687-966X. - ELETTRONICO. - 2017:(2017), pp. 1-9. [10.1155/2017/4790563]

Sex differences of human cardiac progenitor cells in the biological response to TNF-α treatment

PAGANO, FRANCESCA;ANGELINI, FRANCESCO;De Falco, Elena;CAVARRETTA, Elena;La Russa, Raffaele;FRATI, GIACOMO;CHIMENTI, ISOTTA.
Ultimo
2017

Abstract

Adult cardiac progenitor cells (CPCs), isolated as cardiosphere-derived cells (CDCs), represent promising candidates for cardiac regenerative therapy. CDCs can be expanded in vitro manyfolds without losing their differentiation potential, reaching numbers that are appropriate for clinical applications. Since mechanisms of successful CDC survival and engraftment in the damaged myocardium are still critical and unresolved issues, we aimed at deciphering possible key factors capable of bolstering CDC function. In particular, the response and the phenotype of CDCs exposed to low concentrations of the multifunctional cytokine tumor necrosis factor a (TNF-alpha), known to be capable of activating cell survival pathways, have been investigated. Furthermore, differential biological responses of CDCs from male and female donors, in terms of cell cycle progression and cell spreading, have also been assessed. The results obtained indicate that (i) the intracellular signaling activated in our experimental conditions is most likely due to the prosurvival and proliferative signaling of TNF-alpha receptor 2 and that (ii) cells from female patients appear more responsive to TNF-alpha treatment in terms of cell cycle progression and migration ability. In conclusion, the present report highlights the hypothesis that TNF-stimulated CDCs isolated from females may represent a promising candidate for cardiac regenerative therapy applications.
2017
molecular; biology; cell biology
01 Pubblicazione su rivista::01a Articolo in rivista
Sex differences of human cardiac progenitor cells in the biological response to TNF-α treatment / Straface, Elisabetta; Gambardella, Lucrezia; Pagano, Francesca; Angelini, Francesco; Ascione, Barbara; Vona, Rosa; De Falco, Elena; Cavarretta, Elena; La Russa, Raffaele; Malorni, Walter; Frati, Giacomo; Chimenti, Isotta.. - In: STEM CELLS INTERNATIONAL. - ISSN 1687-966X. - ELETTRONICO. - 2017:(2017), pp. 1-9. [10.1155/2017/4790563]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1014801
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