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An ERK-Dependent Feedback Mechanism Prevents Hematopoietic Stem Cell Exhaustion

Cell stem cell.;22(6):879-892.e6. PMID: 29804890
Cell stem cell.;22(6):879-892.e6. PMID: 29804890
123

Hematopoietic stem cells (HSCs) sustain hematopoiesis throughout life. HSCs exit dormancy to restore hemostasis in response to stressful events, such as acute blood loss, and must return to a quiescent state to prevent their exhaustion and resulting bone marrow failure. HSC activation is driven in part through the phosphatidylinositol 3-kinase (PI3K)/AKT/mTORC1 signaling pathway, but less is known about the cell-intrinsic pathways that control HSC dormancy. Here, we delineate an ERK-dependent, rate-limiting feedback mechanism that controls HSC fitness and their re-entry into quiescence. We show that the MEK/ERK and PI3K pathways are synchronously activated in HSCs during emergency hematopoiesis and that feedback phosphorylation of MEK1 by activated ERK counterbalances AKT/mTORC1 activation. Genetic or chemical ablation of this feedback loop tilts the balance between HSC dormancy and activation, increasing differentiated cell output and accelerating HSC exhaustion. These results suggest that MEK inhibitors developed for cancer therapy may find additional utility in controlling HSC activation.

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2021

In vitro reconstitution of Sgk3 activation by phosphatidylinositol 3-phosphate

J Biol Chem 297(2) 100919

D. Pokorny, L. Truebestein, K. D. Fleming, J. E. Burke, and T. A. Leonard

J Biol Chem 297(2) 100919
D. Pokorny, L. Truebestein, K. D. Fleming, J. E. Burke, and T. A. Leonard
2021

Cooperative genetic networks drive embryonic stem cell transition from naïve to formative pluripotency

EMBO J 40:e105776

A. Lackner, R. Sehlke, M. Garmhausen, G. G. Stirparo, M. Huth, F. Titz-Teixeira, P. van der Lelij, J. Ramesmayer, H. F. Thomas, M. Ralser, L. Santini, E. Galimberti, M. Sarov, A. F. Stewart, A. Smith, A. Beyer, and M. Leeb

EMBO J 40:e105776
A. Lackner, R. Sehlke, M. Garmhausen, G. G. Stirparo, M. Huth, F. Titz-Teixeira, P. van der Lelij, J. Ramesmayer, H. F. Thomas, M. Ralser, L. Santini, E. Galimberti, M. Sarov, A. F. Stewart, A. Smith, A. Beyer, and M. Leeb
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