Pathogenic germline IKZF1 variant alters hematopoietic gene expression profiles

Author:

Brodie Seth A.,Khincha Payal P.,Giri Neelam,Bouk Aaron J.,Steinberg Mia,Dai Jieqiong,Jessop Lea,Donovan Frank X.,Chandrasekharappa Settara C.,de Andrade Kelvin C.,Maric Irina,Ellis Steven R.,Mirabello Lisa,Alter Blanche P.,Savage Sharon A.ORCID

Abstract

IKZF1 encodes Ikaros, a zinc finger–containing transcription factor crucial to the development of the hematopoietic system. Germline pathogenic variants in IKZF1 have been reported in patients with acute lymphocytic leukemia and immunodeficiency syndromes. Diamond–Blackfan anemia (DBA) is a rare inherited bone marrow failure syndrome characterized by erythroid hypoplasia, associated with a spectrum of congenital anomalies and an elevated risk of certain cancers. DBA is usually caused by heterozygous pathogenic variants in genes that function in ribosomal biogenesis; however, in many cases the genetic etiology is unknown. We identified a germline IKZF1 variant, rs757907717 C > T, in identical twins with DBA-like features and autoimmune gastrointestinal disease. rs757907717 C > T results in a p.R381C amino acid change in the IKZF1 Ik-x isoform (p.R423C on isoform Ik-1), which we show is associated with altered global gene expression and perturbation of transcriptional networks involved in hematopoietic system development. These data suggest that this missense substitution caused a DBA-like syndrome in this family because of alterations in hematopoiesis, including dysregulation of networks essential for normal erythropoiesis and the immune system.

Publisher

Cold Spring Harbor Laboratory

Subject

General Medicine

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