This work aims to elucidate the relationship between two pathways which play a role both in stem cells and when deregulated in cancer: the pathway of Notch1 (Annu.Rev.Immunol. 23: 945) and the CC Chemokine Receptor 9 (CCR9) signaling. CCR9 is expressed in thymic multipotent precursors (TMP) which have the potentiality to give rise to T, B and dendritic cells (J.Exp.Med. 202: 21). The CCR9 agonist CCL25 is expressed by thymic stromal cells and mediates TMP localization in the thymic sub-capsular zone. CCL25 expression in the gut is also responsible for mature CCR9+ lymphocytes localization at this site and explains relapse location of CCR9+ leukemic cells in the gut (Blood 103: 2806); furthermore CCR9 affects prostate cancer cell migration and invasion (Clinical Cancer Res. 10: 8743). Through the siRNA technique and the use of DAPT, as inhibitor of Notch1 activation, we demonstrated that CCR9 expression in T-ALL cell lines is sustained by Notch1 signaling, and that Notch1 plays a role in CCR9-mediated biological effects such as CCL25-induced chemotaxis and anti-apoptotic effect. This evidence suggests that the integrated activities of these pathways during oncogenesis may allow leukemic stem cells to escape apoptosis and migration at specific sites.
The Notch pathway in tumor cell migration / R. Chiaramonte, L. Mirandola, A. Basile, M. Locati, P. Comi - In: International Workshop on Cancer Stem Cells : Abstracts Book / [a cura di] B. Amati, L. Lanfrancone, S. Minucci, P.G. Pelicci. - Milano : SEMM European School of Medicine, 2005. - pp. 90-90 (( convegno International Workshop on Cancer Stem Cells tenutosi a Milano nel 2005.
The Notch pathway in tumor cell migration
R. ChiaramontePrimo
;L. MirandolaSecondo
;A. Basile;M. LocatiPenultimo
;P. ComiUltimo
2005
Abstract
This work aims to elucidate the relationship between two pathways which play a role both in stem cells and when deregulated in cancer: the pathway of Notch1 (Annu.Rev.Immunol. 23: 945) and the CC Chemokine Receptor 9 (CCR9) signaling. CCR9 is expressed in thymic multipotent precursors (TMP) which have the potentiality to give rise to T, B and dendritic cells (J.Exp.Med. 202: 21). The CCR9 agonist CCL25 is expressed by thymic stromal cells and mediates TMP localization in the thymic sub-capsular zone. CCL25 expression in the gut is also responsible for mature CCR9+ lymphocytes localization at this site and explains relapse location of CCR9+ leukemic cells in the gut (Blood 103: 2806); furthermore CCR9 affects prostate cancer cell migration and invasion (Clinical Cancer Res. 10: 8743). Through the siRNA technique and the use of DAPT, as inhibitor of Notch1 activation, we demonstrated that CCR9 expression in T-ALL cell lines is sustained by Notch1 signaling, and that Notch1 plays a role in CCR9-mediated biological effects such as CCL25-induced chemotaxis and anti-apoptotic effect. This evidence suggests that the integrated activities of these pathways during oncogenesis may allow leukemic stem cells to escape apoptosis and migration at specific sites.
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