multiple therapeutic approaches have been tested in different experimental tumour models and in human cancers. most part of them are based on the hypothesis that the inhibition of tumour growth requires a strong immune response in which a main role is played by CTLs. It is known, however, that an efficient CTL response requires expression of tumour antigens, MHC class I surface molecules presentation, expression of different co-stimulatory molecules and a sustained generation and proliferation of specific cytotoxic CD8+ cells with an efficient CD4+ cooperation. In this context, our group has extensively explored a protocol of combined therapy consisting of the use of chemotherapeutic agents associated with thymosin alpha 1 (Talpha 1) and different cytokines, whose efficacy has been demonstrated in experimental models as well as in human cancers. In this manuscript, the main data supporting a pivotal role of talpha 1 in such combination protocols are reviewed. In particular, a special mention of the molecular mechanisms underlying the effects of talpha 1 on immune effector cells as well as on target tumour cells is provided. these data contribute to explain the mechanism of action of talpha 1, when used in combination therapy, for the treatment of cancer and provide new insights in predicting further possible applications of this peptide in other pathological conditions.

Garaci, E., Pica, F., SINIBALDI VALLEBONA, P., Pierimarchi, P., Mastino, A., Matteucci, C., et al. (2003). Thymosin alpha(1) in combination with cytokines and chemotherapy for the treatment of cancer. INTERNATIONAL IMMUNOPHARMACOLOGY, 3(8), 1145-1150 [10.1016/S1567-5769(03)00053-5].

Thymosin alpha(1) in combination with cytokines and chemotherapy for the treatment of cancer

GARACI, ENRICO;PICA, FRANCESCA
;
SINIBALDI VALLEBONA, PAOLA;MATTEUCCI, CLAUDIA;Rasi, G.
2003-08-01

Abstract

multiple therapeutic approaches have been tested in different experimental tumour models and in human cancers. most part of them are based on the hypothesis that the inhibition of tumour growth requires a strong immune response in which a main role is played by CTLs. It is known, however, that an efficient CTL response requires expression of tumour antigens, MHC class I surface molecules presentation, expression of different co-stimulatory molecules and a sustained generation and proliferation of specific cytotoxic CD8+ cells with an efficient CD4+ cooperation. In this context, our group has extensively explored a protocol of combined therapy consisting of the use of chemotherapeutic agents associated with thymosin alpha 1 (Talpha 1) and different cytokines, whose efficacy has been demonstrated in experimental models as well as in human cancers. In this manuscript, the main data supporting a pivotal role of talpha 1 in such combination protocols are reviewed. In particular, a special mention of the molecular mechanisms underlying the effects of talpha 1 on immune effector cells as well as on target tumour cells is provided. these data contribute to explain the mechanism of action of talpha 1, when used in combination therapy, for the treatment of cancer and provide new insights in predicting further possible applications of this peptide in other pathological conditions.
ago-2003
Pubblicato
Rilevanza internazionale
Articolo
Sì, ma tipo non specificato
Settore MED/07 - MICROBIOLOGIA E MICROBIOLOGIA CLINICA
Settore MEDS-03/A - Microbiologia e microbiologia clinica
English
Con Impact Factor ISI
Animals; Neoplasms; Disease-Free Survival; Humans; Thymosin; Antineoplastic Combined Chemotherapy Protocols; Adjuvants, Immunologic; Cytokines
Garaci, E., Pica, F., SINIBALDI VALLEBONA, P., Pierimarchi, P., Mastino, A., Matteucci, C., et al. (2003). Thymosin alpha(1) in combination with cytokines and chemotherapy for the treatment of cancer. INTERNATIONAL IMMUNOPHARMACOLOGY, 3(8), 1145-1150 [10.1016/S1567-5769(03)00053-5].
Garaci, E; Pica, F; SINIBALDI VALLEBONA, P; Pierimarchi, P; Mastino, A; Matteucci, C; Rasi, G
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/31154
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