| Literature DB >> 27210750 |
Sanaz Manteghi1, Marie-Claude Gingras1, Dmitri Kharitidi1, Luc Galarneau1, Maud Marques2, Ming Yan1, Regina Cencic1, Francis Robert1, Marilène Paquet3, Michael Witcher2, Jerry Pelletier1, Arnim Pause4.
Abstract
Endosomal sorting complexes required for transport (ESCRT) drive cell surface receptor degradation resulting in attenuation of oncogenic signaling and pointing to a tumor suppressor function. Here, we show that loss of function of an ESCRT protein (HD-PTP encoded by the PTPN23 gene, located on the tumor suppressor gene cluster 3p21.3) drives tumorigenesis in vivo. Indeed, Ptpn23(+/-) loss predisposes mice to sporadic lung adenoma, B cell lymphoma, and promotes Myc-driven lymphoma onset, dissemination, and aggressiveness. Ptpn23(+/-)-derived tumors exhibit an unaltered remaining allele and maintain 50% of HD-PTP expression. Consistent with the role of HD-PTP in attenuation of integrin recycling, cell migration, and invasion, hemizygous Ptpn23(+/-) loss increases integrin β1-dependent B cell lymphoma survival and dissemination. Finally, we reveal frequent PTPN23 deletion and downregulation in human tumors that correlates with poor survival. Altogether, we establish HD-PTP/PTPN23 as a prominent haploinsufficient tumor suppressor gene preventing tumor progression through control of integrin trafficking.Entities:
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Year: 2016 PMID: 27210750 DOI: 10.1016/j.celrep.2016.04.076
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423