MNT suppresses T cell apoptosis via BIM and is critical for T lymphomagenesis

Author:

Nguyen Hai Vu,Vandenberg Cassandra J.,Robati Mikara R.,Ng Ashley P.ORCID,Cory SuzanneORCID

Abstract

AbstractThe importance of c-MYC in regulating lymphopoiesis and promoting lymphomagenesis is well-established. Far less appreciated is the vital supporting role of MYC’s relative MNT. Using Rag1Cre-mediated Mnt deletion in lymphoid progenitor cells, we show here that, during normal T cell development, MNT loss enhances apoptosis, at least in part by elevating expression of the pro-apoptotic BH3-only protein BIM. Moreover, using T lymphoma-prone VavP-MYC transgenic mice, we show that Mnt deletion reduces the pool of pre-malignant MYC-driven T lymphoid cells and abrogates thymic T lymphomagenesis. In addition, we establish that Mnt deletion prevents T lymphoma development in γ-irradiated mice, most likely by enhancing apoptosis of T lymphoid cells repopulating the depleted thymus. Taken together with our recent demonstration that MNT is vital for the survival of MYC-driven pre-malignant and malignant B lymphoid cells, these results suggest that MNT represents an important new drug target for both T and B lymphoid malignancies.

Funder

Department of Health | National Health and Medical Research Council

Leukemia and Lymphoma Society

Cancer Council Victoria

State Government of Victoria

Publisher

Springer Science and Business Media LLC

Subject

Cell Biology,Molecular Biology

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