Background: Plex-B1, the receptor of Sema4D, has been implicated in tumour growth, angiogenesis and metastasis. The binding of Sema4D to Plex-B1 can trigger the activation of Met tyrosine kinase, thereby promoting cell dissociation and invasive growth. We tested the hypothesis that the expression of Plex-B1, either alone or in association with Met, can be of predictive value for tumour progression. Methods: The expression and distribution of Plex-B1 and Met were investigated by immunohistochemistry and immunofluorescence in 50 human neoplasias originating in the breast and ovary, and correlated with clinical-pathological data at diagnosis. Results: Plex-B1 and Met were individually expressed in 14% and in 24% of the tumours, respectively. Plex-B1 and Met were co-expressed in 24/50 cases (48%), and in the majority of these (83%) Met was tyrosine phosphorylated. The expression of Plex-B1 or Met alone showed no significant correlation with tumour aggressiveness, whereas advanced stage tumours (III-IV) frequently showed Plex-B1-Met double-positive (9/13). Tumours co-expressing Plex-B1 and Met were characterised by worse grading and higher incidence of lymph node metastases. Out of 22 tumours with lymph node metastases, as many as 19 were Plex-B1 and Met double-positive (p=0.0008), and 17 expressed phosphorylated Met (p=0.002). Conclusion: Plex-B1 assumes a predictive value for unfavourable outcome when co-expressed with Met. © 2009 - IOS Press and the authors. All rights reserved.

Valente, G., Nicotra, G., Arrondini, M., Castino, R., Capparuccia, L., Prat, M., Kerim, S., Tamagnone, L., Isidoro, C., Co-expression of plexin-B1 and Met in human breast and ovary tumours enhances the risk of progression, <<CELLULAR ONCOLOGY>>, 2009; 31 (6): 423-436. [doi:10.3233/CLO-2009-0504] [http://hdl.handle.net/10807/140829]

Co-expression of plexin-B1 and Met in human breast and ovary tumours enhances the risk of progression

Tamagnone, Luca;
2009

Abstract

Background: Plex-B1, the receptor of Sema4D, has been implicated in tumour growth, angiogenesis and metastasis. The binding of Sema4D to Plex-B1 can trigger the activation of Met tyrosine kinase, thereby promoting cell dissociation and invasive growth. We tested the hypothesis that the expression of Plex-B1, either alone or in association with Met, can be of predictive value for tumour progression. Methods: The expression and distribution of Plex-B1 and Met were investigated by immunohistochemistry and immunofluorescence in 50 human neoplasias originating in the breast and ovary, and correlated with clinical-pathological data at diagnosis. Results: Plex-B1 and Met were individually expressed in 14% and in 24% of the tumours, respectively. Plex-B1 and Met were co-expressed in 24/50 cases (48%), and in the majority of these (83%) Met was tyrosine phosphorylated. The expression of Plex-B1 or Met alone showed no significant correlation with tumour aggressiveness, whereas advanced stage tumours (III-IV) frequently showed Plex-B1-Met double-positive (9/13). Tumours co-expressing Plex-B1 and Met were characterised by worse grading and higher incidence of lymph node metastases. Out of 22 tumours with lymph node metastases, as many as 19 were Plex-B1 and Met double-positive (p=0.0008), and 17 expressed phosphorylated Met (p=0.002). Conclusion: Plex-B1 assumes a predictive value for unfavourable outcome when co-expressed with Met. © 2009 - IOS Press and the authors. All rights reserved.
2009
Inglese
Valente, G., Nicotra, G., Arrondini, M., Castino, R., Capparuccia, L., Prat, M., Kerim, S., Tamagnone, L., Isidoro, C., Co-expression of plexin-B1 and Met in human breast and ovary tumours enhances the risk of progression, <<CELLULAR ONCOLOGY>>, 2009; 31 (6): 423-436. [doi:10.3233/CLO-2009-0504] [http://hdl.handle.net/10807/140829]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10807/140829
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