Abstract
NKAP is a multi-functional nuclear protein that has been shown to be essential for hematopoiesis. Deletion of NKAP in hematopoietic stem cells (HSCs) was previously found to result in rapid lethality and hematopoietic failure. NKAP deficient cells also exhibited diminished proliferation and increased expression of the cyclin dependent kinase inhibitors (CDKIs) p19 Ink4d and p21 Cip1. To determine how dysregulation of CDKI expression contributes to the effects of NKAP deficiency, NKAP was deleted in mice also deficient in p19 Ink4d or p21 Cip1 using poly-IC treatment to induce Mx1-cre. Hematopoietic failure and lethality were not prevented by deficiency in either CDKI when NKAP was deleted. Inducible deletion of NKAP in cultured hematopoietic progenitors ex vivo resulted in a senescent phenotype and altered expression of numerous cell cycle regulators including the CDKI p16 INK4a. Interestingly, while combined deficiency in p16 INK4a and p21 Cip1 did not reverse the effect of NKAP deficiency on hematopoiesis in vivo, it did shift the consequence of NKAP deficiency from senescence to apoptosis in ex vivo cultures. These results suggest that NKAP may limit cellular stress that can trigger cell cycle withdrawal or cell death, a role critical for the maintenance of a viable pool of hematopoietic progenitors.
Highlights
Hematopoiesis begins with a small population of hematopoietic stem cell (HSC) in the bone marrow (Sigvardsson, 2009; Matsumoto and Nakayama, 2013)
NKAP is a multifunctional nuclear protein that can act as a transcriptional repressor and Abbreviations: CDK, cyclin dependent kinase; CDKI, cyclin dependent kinase inhibitor; cKO, conditional knockout; dKO, double knockout; ER-cre, estrogen receptor cre; FVD, fixable viability dye; HSC, hematopoietic stem cell; KO, knockout; PARP, poly (ADP-ribose)polymerase; PCNA, proliferating cell nuclear antigen; pH3(S10), serine 10 phosphorylated histone H3; Ub H2A(K119), lysine 119 ubiquitylated histone H2A; WT, wild type
Prior work demonstrated that NKAP is essential for maintenance and survival of HSCs in vivo, and increased expression of p21 Cip1 and p19 Ink4d was observed in NKAP deficient HSCs
Summary
Hematopoiesis begins with a small population of HSCs in the bone marrow (Sigvardsson, 2009; Matsumoto and Nakayama, 2013). Infrequent cell divisions both renew the HSC population and allow differentiation into more proliferative, though uncommitted, types of progenitor cells such as short term HSCs and multipotent progenitors. NKAP is a multifunctional nuclear protein that can act as a transcriptional repressor and Abbreviations: CDK, cyclin dependent kinase; CDKI, cyclin dependent kinase inhibitor; cKO, conditional knockout; dKO, double knockout; ER-cre, estrogen receptor cre; FVD, fixable viability dye; HSC, hematopoietic stem cell; KO, knockout; PARP, poly (ADP-ribose)polymerase; PCNA, proliferating cell nuclear antigen; pH3(S10), serine 10 phosphorylated histone H3; Ub H2A(K119), lysine 119 ubiquitylated histone H2A; WT, wild type
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