Your search keyword '"De Giovanni, Carla"' showing total 3 results

1. HER Tyrosine Kinase Family and Rhabdomyosarcoma: Role in Onset and Targeted Therapy.

Author

De Giovanni, Carla, Landuzzi, Lorena, Palladini, Arianna, Nicoletti, Giordano, Nanni, Patrizia, and Lollini, Pier-Luigi

Subjects

*EPIDERMAL growth factor receptors, *MYOBLASTS, *THERAPEUTICS, *PROTEIN-tyrosine kinases, *TOXINS, *TUMOR growth

Abstract

Rhabdomyosarcomas (RMS) are tumors of the skeletal muscle lineage. Two main features allow for distinction between subtypes: morphology and presence/absence of a translocation between the PAX3 (or PAX7) and FOXO1 genes. The two main subtypes are fusion-positive alveolar RMS (ARMS) and fusion-negative embryonal RMS (ERMS). This review will focus on the role of receptor tyrosine kinases of the human epidermal growth factor receptor (EGFR) family that is comprised EGFR itself, HER2, HER3 and HER4 in RMS onset and the potential therapeutic targeting of receptor tyrosine kinases. EGFR is highly expressed by ERMS tumors and cell lines, in some cases contributing to tumor growth. If not mutated, HER2 is not directly involved in control of RMS cell growth but can be expressed at significant levels. A minority of ERMS carries a HER2 mutation with driving activity on tumor growth. HER3 is frequently overexpressed by RMS and can play a role in the residual myogenic differentiation ability and in resistance to signaling-directed therapy. HER family members could be exploited for therapeutic approaches in two ways: blocking the HER member (playing a driving role for tumor growth with antibodies or inhibitors) and targeting expressed HER members to vehiculate toxins or immune effectors. [ABSTRACT FROM AUTHOR]

Published

2021

2. Bioprofiling TS/A Murine Mammary Cancer for a Functional Precision Experimental Model.

Author

De Giovanni, Carla, Nicoletti, Giordano, Landuzzi, Lorena, Palladini, Arianna, Lollini, Pier-Luigi, and Nanni, Patrizia

Subjects

*BREAST tumors, *CELL lines, *GENE therapy, *GENETIC techniques, *MATHEMATICAL models, *MICE, *TUMOR markers, *THEORY

Abstract

The TS/A cell line was established in 1983 from a spontaneous mammary tumor arisen in an inbred BALB/c female mouse. Its features (heterogeneity, low immunogenicity and metastatic ability) rendered the TS/A cell line suitable as a preclinical model for studies on tumor–host interactions and for gene therapy approaches. The integrated biological profile of TS/A resulting from the review of the literature could be a path towards the description of a precision experimental model of mammary cancer. [ABSTRACT FROM AUTHOR]

Published

2019

3. Cancer Vaccines Co-Targeting HER2/Neu and IGF1R.

Author

De Giovanni, Carla, Landuzzi, Lorena, Palladini, Arianna, Ianzano, Marianna Lucia, Nicoletti, Giordano, Ruzzi, Francesca, Amici, Augusto, Croci, Stefania, Nanni, Patrizia, and Lollini, Pier-Luigi

Subjects

*CANCER vaccines, *ANIMAL experimentation, *CELL lines, *CELL receptors, *EPIDERMAL growth factor, *FLUORESCENT antibody technique, *GENE expression, *MICE, *MUSCLE tumors, *ONCOGENES, *PLASMIDS, *PROTEIN-tyrosine kinases, *RHABDOMYOSARCOMA, *PRECIPITIN tests, *VACCINES, TUMOR prevention

Abstract

(1) Background: Human epidermal growth factor receptor 2 (HER2)/neu-driven carcinogenesis is delayed by preventive vaccines able to elicit autochthonous antibodies against HER2/neu. Since cooperation between different receptor tyrosine kinases (RTKs) can occur in human as well as in experimental tumors, we investigated the set-up of DNA and cell vaccines to elicit an antibody response co-targeting two RTKs: HER2/neu and the Insulin-like Growth Factor Receptor-1 (IGF1R). (2) Methods: Plasmid vectors carrying the murine optimized IGF1R sequence or the human IGF1R isoform were used as electroporated DNA vaccines. IGF1R plasmids were transfected in allogeneic HER2/neu-positive IL12-producing murine cancer cells to obtain adjuvanted cell vaccines co-expressing HER2/neu and IGF1R. Vaccination was administered in the preneoplastic stage to mice prone to develop HER2/neu-driven, IGF1R-dependent rhabdomyosarcoma. (3) Results: Electroporated DNA vaccines for murine IGF1R did not elicit anti-mIGF1R antibodies, even when combined with Treg-depletion and/or IL12, while DNA vaccines carrying the human IGF1R elicited antibodies recognizing only the human IGF1R isoform. Cell vaccines co-expressing HER2/neu and murine or human IGF1R succeeded in eliciting antibodies recognizing the murine IGF1R isoform. Cell vaccines co-targeting HER2/neu and murine IGF1R induced the highest level of anti-IGF1R antibodies and nearly significantly delayed the onset of spontaneous rhabdomyosarcomas. (4) Conclusions: Multi-engineered adjuvanted cancer cell vaccines can break the tolerance towards a highly tolerized RTK, such as IGF1R. Cell vaccines co-targeting HER2/neu and IGF1R elicited low levels of specific antibodies that slightly delayed onset of HER2/neu-driven, IGF1R-dependent tumors. [ABSTRACT FROM AUTHOR]

Published

2019