Long-term Monocyte Dysfunction after Sepsis in Humanized Mice Is Related to Persisted Activation of Macrophage-Colony Stimulation Factor (M-CSF) and Demethylation of PU.1, and It Can Be Reversed by Blocking M-CSF In Vitro or by Transplanting Naïve A

Long-term Monocyte Dysfunction after Sepsis in Humanized Mice Is Related to Persisted Activation of Macrophage-Colony Stimulation Factor (M-CSF) and Demethylation of PU.1, and It Can Be Reversed by Blocking M-CSF In Vitro or by Transplanting Naïve A

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Potential Pitfalls of the Humanized Mice in Modeling Sepsis

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Long-term Monocyte Dysfunction after Sepsis in Humanized Mice Is Related to Persisted Activation of Macrophage-Colony Stimulation Factor (M-CSF) and Demethylation of PU.1, and It Can Be Reversed by Blocking M-CSF In Vitro or by Transplanting Naïve A

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2017 nî lūn-bûn

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2017年論文

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Long-term Monocyte Dysfunction ...... ro or by Transplanting Naïve A

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Long-term Monocyte Dysfunction ...... ro or by Transplanting Naïve A

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Long-term Monocyte Dysfunction ...... ro or by Transplanting Naïve A

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Long-term Monocyte Dysfunction ...... ro or by Transplanting Naïve A

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Long-term Monocyte Dysfunction ...... ro or by Transplanting Naïve A

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Long-term Monocyte Dysfunction ...... Autologous Stem Cells In Vivo

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George S Worthen

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Gwenn Danet-Desnoyers

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Krzysztof Laudanski

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Natalia Lapko

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P2860

Disease tolerance as a defense strategy

Poly(I:C) and Lipopolysaccharide Innate Sensing Functions of Circulating Human Myeloid Dendritic Cells Are Affected In Vivo in Hepatitis C Virus-Infected Patients

Understanding Long-Term Outcomes Following Sepsis: Implications and Challenges

BDCA-2, BDCA-3, and BDCA-4: three markers for distinct subsets of dendritic cells in human peripheral blood

AKT induces transcriptional activity of PU.1 through phosphorylation-mediated modifications within its transactivation domain

Balance of MafB and PU.1 specifies alternative macrophage or dendritic cell fate

The M1 and M2 paradigm of macrophage activation: time for reassessment

Potential autoregulation of transcription factor PU.1 by an upstream regulatory element

Loss of NK stimulatory capacity by plasmacytoid and monocyte-derived DC but not myeloid DC in HIV-1 infected patients.

PU.1 regulates both cytokine-dependent proliferation and differentiation of granulocyte/macrophage progenitors.

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401

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scholarly article

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10.3389/FIMMU.2017.00401

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Mateusz Zawadka

Monika Puzianowska-Kuźnicka

Jacek Polosak

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2017-05-01T00:00:00Z

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28507543

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sepsis

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Long-term Monocyte Dysfunction after Sepsis in Humanized Mice Is Related to Persisted Activation of Macrophage-Colony Stimulation Factor (M-CSF) and Demethylation of PU.1, and It Can Be Reversed by Blocking M-CSF In Vitro or by Transplanting Naïve A

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Long-term Monocyte Dysfunction after Sepsis in Humanized Mice Is Related to Persisted Activation of Macrophage-Colony Stimulation Factor (M-CSF) and Demethylation of PU.1, and It Can Be Reversed by Blocking M-CSF In Vitro or by Transplanting Naïve A

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