Transcription factor B-cell–specific activator protein (BSAP) is differentially expressed in B cells and in subsets of B-cell lymphomas
L Krenacs, AW Himmelmann… - Blood, The Journal …, 1998 - ashpublications.org
L Krenacs, AW Himmelmann, L Quintanilla-Martinez, T Fest, A Riva, A Wellmann, E Bagdi…
Blood, The Journal of the American Society of Hematology, 1998•ashpublications.orgThe paired box containing gene PAX-5 encodes the transcription factor BSAP (B-cell–
specific activator protein), which plays a key role in B-lymphocyte development. Despite its
known involvement in a rare subtype of non-Hodgkin's lymphoma (NHL), a detailed
examination of BSAP expression in NHL has not been previously reported. In this study, we
analyzed normal and malignant lymphoid tissues and cell lines, including 102 cases of B-
cell NHL, 23 cases of T-and null-cell NHL, and 18 cases of Hodgkin's disease. Normal …
specific activator protein), which plays a key role in B-lymphocyte development. Despite its
known involvement in a rare subtype of non-Hodgkin's lymphoma (NHL), a detailed
examination of BSAP expression in NHL has not been previously reported. In this study, we
analyzed normal and malignant lymphoid tissues and cell lines, including 102 cases of B-
cell NHL, 23 cases of T-and null-cell NHL, and 18 cases of Hodgkin's disease. Normal …
Abstract
The paired box containing gene PAX-5 encodes the transcription factor BSAP (B-cell–specific activator protein), which plays a key role in B-lymphocyte development. Despite its known involvement in a rare subtype of non-Hodgkin’s lymphoma (NHL), a detailed examination of BSAP expression in NHL has not been previously reported. In this study, we analyzed normal and malignant lymphoid tissues and cell lines, including 102 cases of B-cell NHL, 23 cases of T- and null-cell NHL, and 18 cases of Hodgkin’s disease. Normal lymphoid tissues showed strong nuclear BSAP expression in mantle zone B cells, less intense reactivity in follicular center B cells, and no expression in cells of the T-cell–rich zones. Monocytoid B cells showed weak expression, whereas plasma cells and extrafollicular large transformed B cells were negative. Of the 102 B-cell NHLs, 83 (81%) demonstrated BSAP expression. All of the 13 (100%) B-cell chronic lymphocytic leukemias (B-CLLs), 21 of (100%) mantle cells (MCLs), and 20 of 21 (95%) follicular lymphomas (FLs) were positive. Moderate staining intensities were found in most B-CLL and FL cases, whereas most MCLs showed strong reactions, paralleling the strong reactivity of nonmalignant mantle cells. Eight of 12 (67%) marginal zone lymphoma cases showed negative or low BSAP levels, and 17 of 24 (71%) large B-cell lymphomas displayed moderate to strong expression. None of the 23 T- and null-cell lymphomas reacted with the BSAP antisera, whereas in Hodgkin’s disease, 2 of 4 (50%) nodular lymphocytic predominance and 5 of 14 (36%) classical cases showed weak nuclear or nucleolar BSAP reactions in a fraction of the tumor cells. Western blot analysis showed a 52-kD BSAP band in B-cell lines, but not in non–B-cell or plasma cell lines. We conclude that BSAP expression is largely restricted to lymphomas of B-cell lineage and that BSAP expression varies in B-cell subsets and subtypes of B-cell NHL. The high levels of BSAP, especially those found in large-cell lymphomas and in some follicular lymphomas, may be a consequence of deregulated gene expression and suggest a possible involvement of PAX-5 in certain B-cell malignancies.
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