Eernstman, Jesse; Veldhuisen, Barbera; Ligthart, Peter; von Lindern, Marieke; van der Schoot, C. Ellen; van den Akker, Emile

doi:10.1038/s41598-021-97149-y

Results

Title: Novel variants in Krueppel like factor 1 that cause persistence of fetal hemoglobin in In(Lu) individuals.
Authors: Eernstman, Jesse; Veldhuisen, Barbera; Ligthart, Peter; von Lindern, Marieke; van der Schoot, C. Ellen; van den Akker, Emile
Abstract: Beta-hemoglobinopathies become prominent after birth due to a switch from γ-globin to the mutated β-globin. Haploinsufficiency for the erythroid specific indispensable transcription factor Krueppel-like factor 1 (KLF1) is associated with high persistence of fetal hemoglobin (HPFH). The In(Lu) phenotype, characterized by low to undetectable Lutheran blood group expression is caused by mutations within KLF1 gene. Here we screened a blood donor cohort of 55 Lutheran weak or negative donors for KLF1 variants and evaluated their effect on KLF1 target gene expression. To discriminate between weak and negative Lutheran expression, a flow cytometry (FCM) assay was developed to detect Lu antigen expression. The Lu(a−b−) (negative) donor group, showing a significant decreased CD44 (Indian blood group) expression, also showed increased HbF and HbA2 levels, with one individual expressing HbF as high as 5%. KLF1 exons and promoter sequencing revealed variants in 80% of the Lutheran negative donors. Thirteen different variants plus one high frequency SNP (c.304 T > C) were identified of which 6 were novel. In primary erythroblasts, knockdown of endogenous KLF1 resulted in decreased CD44, Lu and increased HbF expression, while KLF1 over-expressing cells were comparable to wild type (WT). In line with the pleiotropic effects of KLF1 during erythropoiesis, distinct KLF1 mutants expressed in erythroblasts display different abilities to rescue CD44 and Lu expression and/or to affect fetal (HbF) or adult (HbA) hemoglobin expression. With this study we identified novel KLF1 variants to be include into blood group typing analysis. In addition, we provide further insights into the regulation of genes by KLF1.
Subjects: FETAL hemoglobin; BLOOD donors; PHENOTYPES; HEMOGLOBINS; BLOOD groups
Publication: Scientific Reports, 2021, Vol 11, Issue 1, p1
ISSN: 2045-2322
Publication type: Academic Journal
DOI: 10.1038/s41598-021-97149-y

Novel variants in Krueppel like factor 1 that cause persistence of fetal hemoglobin in In(Lu) individuals.

Eernstman, Jesse; Veldhuisen, Barbera; Ligthart, Peter; von Lindern, Marieke; van der Schoot, C. Ellen; van den Akker, Emile

FETAL hemoglobin; BLOOD donors; PHENOTYPES; HEMOGLOBINS; BLOOD groups

Scientific Reports, 2021, Vol 11, Issue 1, p1

2045-2322

Academic Journal

10.1038/s41598-021-97149-y