Figure 1
Figure 1. Aberrant B cells in cGVHD. (A) Cell surface phenotype of B-cell subsets altered in patients with cGVHD. Most CD27 negative (CD27Neg) B-cell subsets are proportionally decreased in active cGVHD, whereas CD21Lo CD27Neg subsets increase in association with cGVHD activity.44,47 The relative naive B lymphopenia in cGVHD has been associated with a proportional increase in 2 CD27Pos antigen-experienced populations. In contrast, B1 and B10 B-cell subsets are significantly decreased in active cGVHD.42,43 (B) Abnormalities of B-cell homeostasis in different compartments. Aberrant B-cell homeostasis in patients with cGVHD results in abnormal composition of B cells in different sites. B-cell precursors in bone marrow (1). In patients with cGVHD, the production and output of B-cell precursors is decreased. Abnormal composition of B-cell subsets in peripheral blood (2). Both transitional B cells and CD27Neg mature/naive B cells are decreased in frequency in cGVHD. Naive B cells enter secondary lymphoid organs, encounter antigen, and become activated, leading to increased proportions of several B-cell subsets of potential pathological interest. These include the “transitional-like” CD21Lo, the pre-GC IgDHiCD38HiCD27+, and the IgDLoCD38HiCD27Hi populations (all in gray shaded boxes).46 In cGVHD, extrafollicular pre-GC CD27+ B cells and post-GC plasmablast (PB)–like B cells are increased proportionally, whereas immune regulatory B10 cells are decreased. Generation of activated B cells from secondary lymphoid organs (spleen/lymph node) (3). IgDLoCD38HiCD27+ PB-like cells activated in secondary lymphoid tissues produce constitutive IgG and persist in patients with cGVHD who do not respond to B-cell depletion therapy.33

Aberrant B cells in cGVHD. (A) Cell surface phenotype of B-cell subsets altered in patients with cGVHD. Most CD27 negative (CD27Neg) B-cell subsets are proportionally decreased in active cGVHD, whereas CD21Lo CD27Neg subsets increase in association with cGVHD activity.44,47  The relative naive B lymphopenia in cGVHD has been associated with a proportional increase in 2 CD27Pos antigen-experienced populations. In contrast, B1 and B10 B-cell subsets are significantly decreased in active cGVHD.42,43  (B) Abnormalities of B-cell homeostasis in different compartments. Aberrant B-cell homeostasis in patients with cGVHD results in abnormal composition of B cells in different sites. B-cell precursors in bone marrow (1). In patients with cGVHD, the production and output of B-cell precursors is decreased. Abnormal composition of B-cell subsets in peripheral blood (2). Both transitional B cells and CD27Neg mature/naive B cells are decreased in frequency in cGVHD. Naive B cells enter secondary lymphoid organs, encounter antigen, and become activated, leading to increased proportions of several B-cell subsets of potential pathological interest. These include the “transitional-like” CD21Lo, the pre-GC IgDHiCD38HiCD27+, and the IgDLoCD38HiCD27Hi populations (all in gray shaded boxes).46  In cGVHD, extrafollicular pre-GC CD27+ B cells and post-GC plasmablast (PB)–like B cells are increased proportionally, whereas immune regulatory B10 cells are decreased. Generation of activated B cells from secondary lymphoid organs (spleen/lymph node) (3). IgDLoCD38HiCD27+ PB-like cells activated in secondary lymphoid tissues produce constitutive IgG and persist in patients with cGVHD who do not respond to B-cell depletion therapy.33 

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