Your search keyword '"Perin, T"' showing total 9 results

1. Radiotherapy-induced miR-223 prevents relapse of breast cancer by targeting the EGF pathway

Author

Fabris, L, Berton, S, Citron, F, D'Andrea, S, Segatto, I, Nicoloso, M S, Massarut, S, Armenia, J, Zafarana, G, Rossi, S, Ivan, C, Perin, T, Vaidya, J S, Avanzo, M, Roncadin, M, Schiappacassi, M, Bristow, R G, Calin, G, Baldassarre, G, and Belletti, B

Abstract

In breast cancer (BC) patients, local recurrences often arise in proximity of the surgical scar, suggesting that response to surgery may have a causative role. Radiotherapy (RT) after lumpectomy significantly reduces the risk of recurrence. We investigated the direct effects of surgery and of RT delivered intraoperatively (IORT), by collecting irradiated and non-irradiated breast tissues from BC patients, after tumor removal. These breast tissue specimens have been profiled for their microRNA (miR) expression, in search of differentially expressed miR among patients treated or not with IORT. Our results demonstrate that IORT elicits effects that go beyond the direct killing of residual tumor cells. IORT altered the wound response, inducing the expression of miR-223 in the peri-tumoral breast tissue. miR-223 downregulated the local expression of epidermal growth factor (EGF), leading to decreased activation of EGF receptor (EGFR) on target cells and, eventually, dampening a positive EGF–EGFR autocrine/paracrine stimulation loop induced by the post-surgical wound-healing response. Accordingly, both RT-induced miR-223 and peri-operative inhibition of EGFR efficiently prevented BC cell growth and reduced recurrence formation in mouse models of BC. Our study uncovers unknown effects of RT delivered on a wounded tissue and prompts to the use of anti-EGFR treatments, in a peri-operative treatment schedule, aimed to timely treat BC patients and restrain recurrence formation.

Published

2016

2. Chemoendocrine compared with endocrine adjuvant therapies for node-negative breast cancer: predictive value of centrally reviewed expression of estrogen and progesterone receptors--International Breast Cancer Study Group.

Author

Viale G, Regan MM, Maiorano E, Mastropasqua MG, Golouh R, Perin T, Brown RW, Kovács A, Pillay K, Ohlschlegel C, Braye S, Grigolato P, Rusca T, Gelber RD, Castiglione-Gertsch M, Price KN, Goldhirsch A, Gusterson BA, and Coates AS

Published

2008

3. Association of Kaposi's Sarcoma-Associated Herpesvirus-Positive Primary Effusion Lymphoma With Expression of the CD138/Syndecan-1 Antigen

Author

Gaidano, G., Gloghini, A., Gattei, V., Rossi, M.F., Cilia, A.M., Godeas, C., Degan, M., Perin, T., Canzonieri, V., Aldinucci, D., Saglio, G., Carbone, A., and Pinto, A.

Abstract

Primary effusion lymphoma (PEL) represents a novel B-cell non-Hodgkin's lymphoma (NHL) type associated with Kaposi's sarcoma-associated herpesvirus infection and typically growing as lymphomatous effusions in the body cavities. The precise B-cell subset from which PEL originates as well as the biologic mechanisms responsible for its peculiar growth pattern are unclear. In this study, we have analyzed PEL for the expression status of CD138/syndecan-1, a molecule selectively associated with late stages of B-cell differentiation and implicated in cell-to-cell and cell-to-extracellular matrix interactions. PEL patient samples (n = 7) and cell lines (n = 5) were investigated by multiple approaches, including immunocytochemistry, flow cytometry, RNA analysis, and Western blot studies. For comparison, lymphomatous effusions other than PEL (n = 13) and tissue-based NHL (n = 103) were also tested. Expression of CD138/syndecan-1 associates at high frequency with PEL (5 of 7 patient samples and 5 of 5 cell lines), whereas it is consistently absent among other lymphomatous effusions (n = 13). The CD138/syndecan-1 isoform expressed by PEL has an average molecular weight of 420 kD, which is substantially different from that of CD138/syndecan-1 molecules generally expressed by plasma cells. These data, along with previous immunophenotypic evidence, unequivocally define that PEL cells represent a preterminal stage of B-cell differentiation and may bear implications for the peculiar growth pattern of this lymphoma.

Published

1997

4. Lower confidence limit for the availability of a prrallel system with renwable components

Author

perin, T. El and Gertsbakh, I.

Abstract

A parallel system of n independent and renewable components with exponential up and down times is considered, A conservative lower confidence limit (LCL) on its availability in equilibrium is constructed by using the maximization method suggested by Gnedenko et al. (1969). The empirical coverage of the LCL is investigated by using the Monte Carlo simulation technique. The method uses the empirical percentage points of the sums of independent random variables distributed according to the F-distribution. A comparison is done with an alternative method of Zacks (1987) based on a large sample normal approximation. It is shown that the maximization method performs better than the large sample normal approximation.

Published

1988

5. Association of Kaposi's Sarcoma-Associated Herpesvirus-Positive Primary Effusion Lymphoma With Expression of the CD138/Syndecan-1 Antigen

Author

Gaidano, G., Gloghini, A., Gattei, V., Rossi, M.F., Cilia, A.M., Godeas, C., Degan, M., Perin, T., Canzonieri, V., Aldinucci, D., Saglio, G., Carbone, A., and Pinto, A.

Abstract

Primary effusion lymphoma (PEL) represents a novel B-cell non-Hodgkin's lymphoma (NHL) type associated with Kaposi's sarcoma-associated herpesvirus infection and typically growing as lymphomatous effusions in the body cavities. The precise B-cell subset from which PEL originates as well as the biologic mechanisms responsible for its peculiar growth pattern are unclear. In this study, we have analyzed PEL for the expression status of CD138/syndecan-1, a molecule selectively associated with late stages of B-cell differentiation and implicated in cell-to-cell and cell-to-extracellular matrix interactions. PEL patient samples (n = 7) and cell lines (n = 5) were investigated by multiple approaches, including immunocytochemistry, flow cytometry, RNA analysis, and Western blot studies. For comparison, lymphomatous effusions other than PEL (n = 13) and tissue-based NHL (n = 103) were also tested. Expression of CD138/syndecan-1 associates at high frequency with PEL (5 of 7 patient samples and 5 of 5 cell lines), whereas it is consistently absent among other lymphomatous effusions (n = 13). The CD138/syndecan-1 isoform expressed by PEL has an average molecular weight of 420 kD, which is substantially different from that of CD138/syndecan-1 molecules generally expressed by plasma cells. These data, along with previous immunophenotypic evidence, unequivocally define that PEL cells represent a preterminal stage of B-cell differentiation and may bear implications for the peculiar growth pattern of this lymphoma.

Published

1997

6. Intraoperative radiotherapy during breast-conserving surgery: 10-year of our experience.

Author

Mileto, M., Perin, T., Trovo', M., Roncadin, M., Capra, E., Avanzo, M., and Massarut, S.

Subjects

CANCER radiotherapy, LUMPECTOMY, PERIOPERATIVE care, ANESTHESIA, X-rays

Published

2016

7. P259 TARGIT modulates miRNAs expression to control growth factors production in breast tissue.

Author

Belletti, B., Massarut, S., D'Andrea, S., Martinuzzo, D., Roncadin, M., Perin, T., Sartor, G., Trovò, M.G., Calin, G., and Baldassarre, G.

Published

2011

8. 102 How the 70-gene tumour expression profile “MammaPrint” can assist in St Gallen 2009 treatment recommendations in 12 Italian hospitals

Author

Zanconati, F.Q.P., Sapino, A., Di Bonito, M., Perin, T., Pronzato, P., Giardina, C., Tinterri, C., Generali, D., Gangi, S.S., and Di Napoli, A.

Published

2010

9. Immunohistochemical evaluation of multiple biological markers in ductal carcinoma in situ of the breast

Author

Perin, T

Published

1996