Structural variations involving MYC in BL. Translocations between the MYC locus (chromosome 8) and the IGH (chromosome 14), IGK (chromosome 2), or IGL (chromosome 22) loci in tumors with IG-MYC breakpoints detected from WGS (N = 212). The subset of IGH-MYC breakpoints with high-confidence breakpoint positions identified are colored on the basis of their category, as determined by location within IGH (red = CSR, or blue = SHM). Bar charts on the lower left display the frequency of IG-MYC breakpoints (left) and IGH breakpoint category (right). The lower part of A and B linearly depicts IGH-MYC rearrangements colored by breakpoint category. (A) Adult (N = 80) and pediatric (N = 132) samples are shown separately. (B) EBV-negative (N = 103) and EBV-positive (N = 109) samples are shown separately. The inferred IGH breakpoint category frequencies stratified by age (C) and EBV status (D) were subjected to a Fisher exact test (∗∗P < .01). (E) AICDA expression in adult and pediatric BL tumors separated by EBV status (Wilcoxon rank sum test; ∗∗∗P < .001). AICDA, activation-induced cytidine deaminase; CSR, class-switch recombination; IGH, immunoglobulin heavy chain; IGK, immunoglobulin light chain kappa; IGL, immunoglobulin light chain lambda; SHM, somatic hypermutation.
Figure 1.

Structural variations involving MYC in BL. Translocations between the MYC locus (chromosome 8) and the IGH (chromosome 14), IGK (chromosome 2), or IGL (chromosome 22) loci in tumors with IG-MYC breakpoints detected from WGS (N = 212). The subset of IGH-MYC breakpoints with high-confidence breakpoint positions identified are colored on the basis of their category, as determined by location within IGH (red = CSR, or blue = SHM). Bar charts on the lower left display the frequency of IG-MYC breakpoints (left) and IGH breakpoint category (right). The lower part of A and B linearly depicts IGH-MYC rearrangements colored by breakpoint category. (A) Adult (N = 80) and pediatric (N = 132) samples are shown separately. (B) EBV-negative (N = 103) and EBV-positive (N = 109) samples are shown separately. The inferred IGH breakpoint category frequencies stratified by age (C) and EBV status (D) were subjected to a Fisher exact test (∗∗P < .01). (E) AICDA expression in adult and pediatric BL tumors separated by EBV status (Wilcoxon rank sum test; ∗∗∗P < .001). AICDA, activation-induced cytidine deaminase; CSR, class-switch recombination; IGH, immunoglobulin heavy chain; IGK, immunoglobulin light chain kappa; IGL, immunoglobulin light chain lambda; SHM, somatic hypermutation.

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