4.7 Article

An ELF4 hypomorphic variant results in NK cell deficiency

Journal

JCI INSIGHT
Volume 7, Issue 23, Pages -

Publisher

AMER SOC CLINICAL INVESTIGATION INC
DOI: 10.1172/jci.insight.155481

Keywords

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Funding

  1. NIH [S10OD026845, R01 AI120989, AI067946, R01 AI137275, T32 GM007367, R25 GM056929, T32 GM088129, AI120989S1, T32 GM008280]
  2. NIH National Human Genome Research Institute/National Heart, Lung, and Blood Institute [UM1 HG006542]
  3. BCM-GREGoR [U01 HG011758]
  4. NIH National Cancer Institute [R01 CA207086-01A]
  5. ASH Bridge Award
  6. National Human Genome Research Institute [K08 HG008986]
  7. Welch Foundation [Q0035, R01 EY026545]

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NK cell deficiencies are a type of primary immune deficiency that affect the number, maturity, or function of NK cells. Patients with NKD are more susceptible to viral infections and may experience chronic, recurrent, and fatal infections. This study identified a damaging variant in the ELF4 gene as a potentially novel cause of NKD.
NK cell deficiencies (NKD) are a type of primary immune deficiency in which the major immunologic abnormality affects NK cell number, maturity, or function. Since NK cells contribute to immune defense against virally infected cells, patients with NKD experience higher susceptibility to chronic, recurrent, and fatal viral infections. An individual with recurrent viral infections and mild hypogammaglobulinemia was identified to have an X-linked damaging variant in the transcription factor gene ELF4. The variant does not decrease expression but disrupts ELF4 protein interactions and DNA binding, reducing transcriptional activation of target genes and selectively impairing ELF4 function. Corroborating previous murine models of ELF4 deficiency (Elf4-/-) and using a knockdown human NK cell line, we determined that ELF4 is necessary for normal NK cell development, terminal maturation, and function. Through characterization of the NK cells of the proband, expression of the proband's variant in Elf4-/- mouse hematopoietic precursor cells, and a human in vitro NK cell maturation model, we established this ELF4 variant as a potentially novel cause of NKD.

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