Science and Research

Limited role of interferon-kappa (IFNK) truncating mutations in common variable immunodeficiency

We used whole exome sequencing to determine the genetic background of CVID in two non-consanguineous German families. We identified IFNK (interferon-kappa) as the only candidate gene that harbored truncating mutations in affected members from both families. One family segregated c.30_31insTGTT, a known frameshift variant, while the other family segregated the novel IFNK mutation p.K199X that creates a premature stop codon. We sequenced the whole coding region of IFNK in a further series of 167 CVID patients and 192 healthy controls. Frameshift mutation c.30_31insTGTT was identified in 12 cases and 17 controls (OR 0.79, 95% CI 0.33-1.81, p=0.79), whereas the p.K199X mutation remained restricted to the original family. No additional truncating variants were found. We conclude that, given their frequent occurrence in non-diseased family members and controls, it is unlikely that truncating variants in IFNK constitute a major factor in the development of CVID.

  • Atschekzei, F.; Dork, T.; Schurmann, P.; Geffers, R.; Witte, T.; Schmidt, R. E.

Keywords

  • Common variable immunodeficiency (CVID)
  • Interferon kappa gene (IFNK)
  • Whole exome sequencing
Publication details
DOI: 10.1016/j.cyto.2017.03.005
Journal: Cytokine
Pages: 71-74 
Work Type: Original
Location: BREATH
Disease Area: General Lung and Other
Partner / Member: MHH
Access-Number: 28324805

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