Selected article for: "antiviral immunity and respiratory infection"

Author: Geng, Tingting; Yang, Duomeng; Lin, Tao; Harrison, Andrew G.; Wang, Binsheng; Torrance, Blake; Wang, Kepeng; Wang, Yanlin; Yang, Long; Haynes, Laura; Cheng, Gong; Vella, Anthony T.; Fikrig, Erol; Wang, Penghua
Title: An Essential Role of UBXN3B in B Lymphopoiesis
  • Cord-id: l7aj1jpk
  • Document date: 2021_8_24
  • ID: l7aj1jpk
    Snippet: Hematopoiesis is finely regulated to enable timely production of the right numbers and types of mature immune cells to maintain tissue homeostasis. Dysregulated hematopoiesis may compromise antiviral immunity and/or exacerbate immunopathogenesis. Herein, we report an essential role of UBXN3B in maintenance of hematopoietic homeostasis and restriction of immunopathogenesis during respiratory viral infection. Ubxn3b deficient (Ubxn3b−/−) mice are highly vulnerable to SARS-CoV-2 and influenza A
    Document: Hematopoiesis is finely regulated to enable timely production of the right numbers and types of mature immune cells to maintain tissue homeostasis. Dysregulated hematopoiesis may compromise antiviral immunity and/or exacerbate immunopathogenesis. Herein, we report an essential role of UBXN3B in maintenance of hematopoietic homeostasis and restriction of immunopathogenesis during respiratory viral infection. Ubxn3b deficient (Ubxn3b−/−) mice are highly vulnerable to SARS-CoV-2 and influenza A infection, characterized by more severe lung immunopathology, lower virus-specific IgG, significantly fewer B cells, but more myeloid cells than Ubxn3b+/+ littermates. This aberrant immune compartmentalization is recapitulated in uninfected Ubxn3b−/− mice. Mechanistically, UBXN3B controls precursor B-I (pre-BI) transition to pre-BII and subsequent proliferation in a cell-intrinsic manner, by maintaining BLNK protein stability and pre-BCR signaling. These results reveal an essential role of UBXN3B for the early stage of B cell development.

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