TY - JOUR
T1 - GFAP-Cre-mediated transgenic activation of Bmi1 results in pituitary tumors
AU - Westerman, Bart A.
AU - Blom, Marleen
AU - Tanger, Ellen
AU - van der Valk, Martin
AU - Song, Ji Ying
AU - van Santen, Marije
AU - Gadiot, Jules
AU - Cornelissen-Steijger, Paulien
AU - Zevenhoven, John
AU - Prosser, Haydn M.
AU - Uren, Anthony
AU - Aronica, Eleonora
AU - van Lohuizen, Maarten
PY - 2012/5/4
Y1 - 2012/5/4
N2 - Bmi1 is a member of the polycomb repressive complex 1 and plays different roles during embryonic development, depending on the developmental context. Bmi1 over expression is observed in many types of cancer, including tumors of astroglial and neural origin. Although genetic depletion of Bmi1 has been described to result in tumor inhibitory effects partly through INK4A/Arf mediated senescence and apoptosis and also through INK4A/Arf independent effects, it has not been proven that Bmi1 can be causally involved in the formation of these tumors. To see whether this is the case, we developed two conditional Bmi1 transgenic models that were crossed with GFAP-Cre mice to activate transgenic expression in neural and glial lineages. We show here that these mice generate intermediate and anterior lobe pituitary tumors that are positive for ACTH and beta-endorphin. Combined transgenic expression of Bmi1 together with conditional loss of Rb resulted in pituitary tumors but was insufficient to induce medulloblastoma therefore indicating that the oncogenic function of Bmi1 depends on regulation of p16INK4A/Rb rather than on regulation of p19ARF/p53. Human pituitary adenomas show Bmi1 overexpression in over 50% of the cases, which indicates that Bmi1 could be causally involved in formation of these tumors similarly as in our mouse model.
AB - Bmi1 is a member of the polycomb repressive complex 1 and plays different roles during embryonic development, depending on the developmental context. Bmi1 over expression is observed in many types of cancer, including tumors of astroglial and neural origin. Although genetic depletion of Bmi1 has been described to result in tumor inhibitory effects partly through INK4A/Arf mediated senescence and apoptosis and also through INK4A/Arf independent effects, it has not been proven that Bmi1 can be causally involved in the formation of these tumors. To see whether this is the case, we developed two conditional Bmi1 transgenic models that were crossed with GFAP-Cre mice to activate transgenic expression in neural and glial lineages. We show here that these mice generate intermediate and anterior lobe pituitary tumors that are positive for ACTH and beta-endorphin. Combined transgenic expression of Bmi1 together with conditional loss of Rb resulted in pituitary tumors but was insufficient to induce medulloblastoma therefore indicating that the oncogenic function of Bmi1 depends on regulation of p16INK4A/Rb rather than on regulation of p19ARF/p53. Human pituitary adenomas show Bmi1 overexpression in over 50% of the cases, which indicates that Bmi1 could be causally involved in formation of these tumors similarly as in our mouse model.
UR - http://www.scopus.com/inward/record.url?scp=84860535452&partnerID=8YFLogxK
U2 - 10.1371/journal.pone.0035943
DO - 10.1371/journal.pone.0035943
M3 - Article
C2 - 22574128
AN - SCOPUS:84860535452
VL - 7
JO - PLoS ONE
JF - PLoS ONE
SN - 1932-6203
IS - 5
M1 - e35943
ER -