T-cell non-Hodgkin's lymphomas can be considered the neoplastic equivalents of immunologically functional, site-restricted T lymphocytes. Little is known about the occurrence and clinical behavior of T-cell lymphomas that are the neoplastic equivalents of different functional T-cell subsets. Here, we investigated the prevalence, preferential site, immunophenotype, and clinical behavior of the neoplastic equivalents of activated cytotoxic T cells (CTLs) in a group of 140 nodal and extranodal T-cell lymphomas. Activated CTLs were shown immunohistochemically with a monoclonal antibody against granzyme B, a major constituent of the cytotoxic granules of activated T cells. Granzyme B-positive T-cell lymphomas were mainly found in mucosa- associated lymphoid tissue (MALT; nose, 63% of the cases; gastrointestinal tract, 46%; and lung, 33%). Granzyme B-positive cases with primary localization in MALT were more often associated with angioinvasion (P = .005), necrosis (P = .002), and histologic characteristics of celiac disease in adjacent mucosa not involved with lymphoma. Eosinophilia was more often observed in granzyme B-negative cases (P = .03). Most cases belonged to the pleomorphic medium- and large-cell group of the Kiel classification. CD30 expression was more often found in granzyme B-positive lymphomas of MALT (P = .04), whereas CD56 expression was exclusively found in nasal granzyme B-positive lymphomas. Immunophenotypically, most of the cases should be considered as neoplastic equivalents of activated CTLs based on the presence of T- cell markers on tumor cells. In two cases of nasal lymphoma, tumor cells probably were the neoplastic counterparts of natural killer cells. The prognosis of the granzyme B-positive gastrointestinal T-cell lymphomas was poor but did not differ from granzyme B-negative gastrointestinal T-cell lymphomas. This indicates that, in peripheral T- cell lymphomas, site of origin is more important as a prognostic parameter than derivation of activated CTLs.
ARTICLES|
December 1, 1994
Granzyme B-expressing peripheral T-cell lymphomas: neoplastic equivalents of activated cytotoxic T cells with preference for mucosa- associated lymphoid tissue localization
PC de Bruin,
PC de Bruin
Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.
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JA Kummer,
JA Kummer
Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.
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P van der Valk,
P van der Valk
Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.
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P van Heerde,
P van Heerde
Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.
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PM Kluin,
PM Kluin
Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.
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R Willemze,
R Willemze
Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.
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GJ Ossenkoppele,
GJ Ossenkoppele
Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.
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T Radaszkiewicz,
T Radaszkiewicz
Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.
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CJ Meijer
CJ Meijer
Department of Pathology, Free University Hospital, Amsterdam, The Netherlands.
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Blood (1994) 84 (11): 3785–3791.
Citation
PC de Bruin, JA Kummer, P van der Valk, P van Heerde, PM Kluin, R Willemze, GJ Ossenkoppele, T Radaszkiewicz, CJ Meijer; Granzyme B-expressing peripheral T-cell lymphomas: neoplastic equivalents of activated cytotoxic T cells with preference for mucosa- associated lymphoid tissue localization. Blood 1994; 84 (11): 3785–3791. doi: https://doi.org/10.1182/blood.V84.11.3785.bloodjournal84113785
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