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Corticomedullary differentiation and maturational arrest in thymomas
Author(s) -
Ströbel Philipp,
Hartmann Elena,
Rosenwald Andreas,
Kalla Jörg,
Ott German,
Friedel Godehard,
Schalke Berthold,
Kasahara Masanori,
Tomaru Utano,
Marx Alexander
Publication year - 2014
Publication title -
histopathology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.626
H-Index - 124
eISSN - 1365-2559
pISSN - 0309-0167
DOI - 10.1111/his.12279
Subject(s) - thymoma , pathology , medullary cavity , biology , cytokeratin , immunohistochemistry , lineage (genetic) , intermediate filament , cellular differentiation , anatomy , medicine , cell , cytoskeleton , biochemistry , gene , genetics
Aims Morphological complexity hampers the histological classification of thymomas. Our aim was to determine whether the use of novel differentiation and maturation markers of cortical and medullary thymic epithelial cells (c TEC s and m TEC s) might provide an approach to understanding the underlying biology of these tumours. Methods and results Fifty‐seven thymomas were studied by immunohistochemistry. The cortical markers used were B 5 T , PRSS 16, and cathepsin V. The medullary markers used were CD40, claudin‐4, AIRE , and desmin. Involucrin and cytokeratin 10 were used to study terminal mTEC maturation. Irrespective of histological subtype, most thymomas contained distinct areas with cortical and medullary differentiation. Type B1, type B2 and type AB thymomas showed marked bi‐lineage differentiation, with lack of terminal m TEC maturation in type AB. Type AB thymomas were unique in showing areas where cells with either cortical or medullary differentiation were intimately ‘mixed’ at the single‐cell level. Type B3 and type A thymomas showed only abortive lineage differentiation and maturation. Conclusions Thymomas show highly characteristic patterns of bi‐lineage TEC differentiation that reflect the histological subtypes recognized by the WHO classification. We hypothesize that thymomas arise from thymic precursor cells with different cortical and/or medullary maturation defects.

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