FigureĀ 4.
NFE2 somatic mutations in FPDMM and hematologic malignancies. (A) Lollipop plot of NFE2 somatic mutations in NIH FPDMM cohort. Based on ACMG criteria, both nonsense mutations are LP (p.Leu57ArgfsTer27: PVS1 and PM2; p.Gln324Ter: PVS1 and PM2). The missense mutation, p.Asn276His, is considered as a VUS (PP3, PM2, and BP1) based on the PhyloP100way score but pathogenic according to in silico prediction (P/LP: 21/27; uncertain: 6/27). (B) Somatic alteration frequency of NFE2 gene in AACR GENIE data set and cBioportal myeloid neoplasm data set. (C) ChIP-seq data on RUNX1 binding in NFE2 locus in CD34+ cells from 4 publicly available data sets.37-39 Binding profile data were downloaded from CODEX database.40 AACR GENIE, American Association for Cancer Research Genomics Evidence Neoplasia Information Exchange; HSPCs, hematopoietic stem and progenitor cells; UCB, umbilical cord blood.

NFE2 somatic mutations in FPDMM and hematologic malignancies. (A) Lollipop plot of NFE2 somatic mutations in NIH FPDMM cohort. Based on ACMG criteria, both nonsense mutations are LP (p.Leu57ArgfsTer27: PVS1 and PM2; p.Gln324Ter: PVS1 and PM2). The missense mutation, p.Asn276His, is considered as a VUS (PP3, PM2, and BP1) based on the PhyloP100way score but pathogenic according to in silico prediction (P/LP: 21/27; uncertain: 6/27). (B) Somatic alteration frequency of NFE2 gene in AACR GENIE data set and cBioportal myeloid neoplasm data set. (C) ChIP-seq data on RUNX1 binding in NFE2 locus in CD34+ cells from 4 publicly available data sets.37-39 Binding profile data were downloaded from CODEX database.40 AACR GENIE, American Association for Cancer Research Genomics Evidence Neoplasia Information Exchange; HSPCs, hematopoietic stem and progenitor cells; UCB, umbilical cord blood.

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