Elena Sironi
University of Milan
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Publication
Featured researches published by Elena Sironi.
Oncogene | 2000
Silvia Maria Sirchia; Anne T. Ferguson; Elena Sironi; Smitha Subramanyan; Rosaria Orlandi; Saraswati Sukumar; Nicoletta Sacchi
Retinoic acid (RA)-resistance in breast cancer cells has been associated with irreversible loss of retinoic acid receptor β, RARβ, gene expression. Search of the causes affecting RARβ gene activity has been oriented at identifying possible differences either at the level of one of the RARβ promoters, RARβ2, or at regulatory factors. We hypothesized that loss of RARβ2 activity occurs as a result of multiple factors, including epigenetic modifications, which can pattern RARβ2 chromatin state. Using methylation-specific PCR, we found hypermethylation at RARβ2 in a significant proportion of both breast cancer cell lines and primary breast tumors. Treatment of cells with a methylated RARβ2 promoter, by means of the DNA methyltransferase inhibitor 5-Aza-2′-deoxycytidine (5-Aza-CdR), led to demethylation within RARβ2 and expression of RARβ indicating that DNA methylation is at least one factor, contributing to RARβ inactivity. However, identically methylated promoters can differentially respond to RA, suggesting that RARβ2 activity may be associated to different repressive chromatin states. This supposition is supported by the finding that the more stable repressive RARβ2 state in the RA-resistant MDA-MB-231 cell line can be alleviated by the HDAC inhibitor, trichostatin A (TSA), with restoration of RA-induced RARβ transcription. Thus, chromatin-remodeling drugs might provide a strategy to restore RARβ activity, and help to overcome the hurdle of RA-resistance in breast cancer.
Journal of Cutaneous Pathology | 2004
Elena Sironi; Amilcare Cerri; Dario Tomasini; Silvia Maria Sirchia; Giovanni Porta; F. Rossella; Francesca Romana Grati; Giuseppe Simoni
Background: Studies on basal cell carcinoma (BCC) have demonstrated that patched gene and p53 gene located at 9q22.3 and 17p13 are the main genes responsible for the onset of this tumor. In order to identify a possible involvement of other tumor suppressor genes, we screened 19 cases of BCCs for loss of heterozygosity (LOH).
Cancer Genetics and Cytogenetics | 2000
Francesca Romana Grati; Silvia Maria Sirchia; Isabella Garagiola; Elena Sironi; Silvestre Galioto; F. Rossella; Paola Serafini; Francesca Dulcetti; Alberto Bozzetti; Roberto Brusati; Giuseppe Simoni
We analyzed 25 oral and oropharyngeal epithelial carcinomas for loss of heterozygosity (LOH) and microsatellite instability by using 55 oligonucleotide repeat markers located in 45 chromosomal regions. The aim was to identify which chromosomal regions and tumor-suppressor genes (TSGs) are preferentially lost in these tumors and to relate LOH at specific loci to clinicopathologic data. The analysis was performed on tumor tissue and on a corresponding normal tissue (blood lymphocytes) with the use of the polymerase chain reaction technique followed by microsatellite allele separation with denaturing gel electrophoresis. Thirty-two of 45 chromosomal regions demonstrated a significant (>/=20%) incidence of LOH. An allelic loss of >/=50% was found in 9p21 (77.8%), 8p22-23 (70%), 3p12 (61.5%), 1p36.1 and 12q22 (60%), 3q28 (57.1%), 5q23.3 (54.5%), 3p25-26, 3p24, and 7q35 (50%). We did not find any microsatellite instability. Our results suggest that in addition to a group of TSGs, pleiotropic for several tumor types, other suppressor genes are specifically involved in oral and oropharyngeal carcinogenesis.
Cancer Genetics and Cytogenetics | 2000
Silvia Maria Sirchia; Elena Sironi; Francesca Romana Grati; Paola Serafini; Isabella Garagiola; F. Rossella; Francesca Dulcetti; Giorgio Pardi; Salvatore Garsia; Giuseppe Simoni
We analyzed 37 samples of endometrial adenocarcinoma for loss of heterozygosity (LOH) by using a panel of 44 microsatellites located in 29 chromosomal regions. The aim of our study was to investigate the existence of a possible preferential involvement of some tumor suppressor genes in endometrial carcinogenesis. The analysis was performed on tumoral tissue and on a corresponding normal tissue by the use of polymerase chain reaction (PCR) and the comparison of the amplified alleles. We observed significative LOH (>20%) in the chromosomal regions of 2q14 (33.33%), 7q35 (24.00%), 10q22.1 (37. 50%), 11q13-q14 (44.12%), 15q26 (40.63%), 17p13 (25.71%), and 17q21. 3 (37.04%). We defined a 1-cM minimal common deletion in 11q13-q14 between D11S911 and D11S937 markers. A statistical analysis revealed a positive correlation between LOH of 11q13-q14 and clinicopathological data.
Atherosclerosis | 2001
Francesca Romana Grati; Giorgio Ghilardi; Silvia Maria Sirchia; Federico Massaro; Barbara Cassani; Roberto Scorza; Chiara De Andreis; Elena Sironi; Giuseppe Simoni
We have investigated 28 atherosclerotic plaques of human carotid arteries with a panel of 39 microsatellite markers for the presence of LOH. The objective of this research was to verify if LOH, described in association with tumorigenic process, could be involved also in benign fibroproliferative disease. Seventy percent of samples demonstrated allelic imbalance: 50% of cases showed LOH at a minimum of one locus, 3.5% at a minimum of two loci and 14.3% at three or more loci. The percentages of LOH ranged between 3.8 and 14.3% and the highest involved polymorphic marker is the NOS3 internal dinucleotide repeat. Our results indicate that, like tumorigenesis, the atherogenic process could also involve LOH mechanism. Furthermore, the finding regarding the NOS3 internal polymorphism suggests a possible role of the gene as cofactor in formation of the atheromas.
Cereal Chemistry | 2001
Elena Sironi; Nicoletta Guerrieri
ABSTRACT The surface properties of glutens isolated from a durum wheat cultivar (Capeiti) and two bread wheats (Riband and Hereward) were investigated using intrinsic and extrinsic fluorescence. Intrinsic fluorescence decreased on increasing protein concentration and increased after urea addition. The extrinsic fluorescence was evaluated by a titration with 8-anilino-1-naphthalene sulphonate (ANS), an hydrophobic probe. The saturating concentration for ANS and its dissociation constant (Kd) were determined. The hydrophobicity of durum and bread wheat gluten showed a different behavior increasing the protein concentration: Capeiti was not influenced, but there was a change on the gluten surface for Riband and Hereward. The significance in understanding gluten structure and the relevance of the surface properties are discussed.
Cancer Research | 2002
Silvia Maria Sirchia; Mingqiang Ren; Roberto Pili; Elena Sironi; Giulia Somenzi; Riccardo Ghidoni; Salvatore Toma; Guido Nicolò; Nicoletta Sacchi
Journal of Agricultural and Food Chemistry | 2005
Chiara Magni; Anita Herndl; Elena Sironi; Alessio Scarafoni; Cinzia Ballabio; Patrizia Restani; Roberto Bernardini; Elio Novembre; and Alberto Vierucci; Marcello Duranti
Journal of Agricultural and Food Chemistry | 2005
Chiara Magni; Cinzia Ballabio; Patrizia Restani; Elena Sironi; Alessio Scarafoni; Claudio Poiesi; Marcello Duranti
European Food Research and Technology | 2005
Elena Sironi; Fabio Sessa; Marcello Duranti
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Fondazione IRCCS Ca' Granda Ospedale Maggiore Policlinico
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