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Publication
Featured researches published by Brian P Eyden.
Virchows Archiv | 1992
Brian P Eyden; R. J. Hale; I. Richmond; C. H. Buckley
The filamentous components of the cytoskeleton in smooth muscle cells of leiomyomata and normal myometrium were studied by immunohistochemistry and electron microscopy. Fourteen patients hysterectomised for non-malignant disease provided leiomyomata of conventional histological type and histologically normal myometrium: four samples of fetal myometrium were studied by immunohistochemistry alone. All samples of leiomyoma and myometrium were strongly positive for α-smooth muscle actin and desmin, the latter often as paranuclear columns or granules. Vimentin was also stained in most samples but less intensely, while cytokeratin stained in about half the samples with an intensity comparable to that of vimentin. By electron microscopy, myofilaments with focal densities were abundant in both normal myometrium and leiomyomata. Intermediate filaments corresponding to the desmin and vimentin demonstrated by immunohistochemistry were also recognised in a variety of architectural arrangements. At one extreme, comparatively small numbers of filaments were loosely distributed around membranous organelles; at the other, filaments formed conspicuous aggregates, largely excluding other organelles and corresponding to the paranuclear granules seen by immunohistochemistry. A comparison of these findings with those of the literature and comments on the possible significance and origin of these aggregates are provided.
Virchows Archiv | 2002
Takuya Aoki; Hajime Okita; Hidekazu Kayano; Hideki Orikasa; Kentaro Watanabe; Brian P Eyden; Kazuto Yamazaki
A case of plasmacytoma of the pleural cavity is reported with massive malignant pleural effusion, which, most unusually, lacked monoclonal gammopathy, thereby making it difficult to distinguish from lymphoma. The pleural tumor and pleural effusion contained large mononuclear lymphoma-like cells with distinct nucleoli. Immunohistochemistry revealed neither lymphoma markers nor clonal cytoplasmic nor cell surface immunoglobulins. Tumor cells were stained with vimentin and the plasma cell markers, VS38c, CD138 (syndecan-1), and MUM1 antibodies. Bone marrow contained small amounts of tumor consisting of similar cells. Electron microscopy showed well developed rough endoplasmic reticulum and peripherally positioned nuclei with euchromatin. Flow cytometry of bone marrow revealed a minimal involvement of CD38-positive cells. Chromosomal analysis of marrow cells revealed a complex abnormal karyotype. A polymerase chain reaction demonstrated clonal re-arrangement of the immunoglobulin heavy-chain gene. The overall results indicate a clonal expansion of tumor cells with primitive plasma cell differentiation with the highly unusual feature of absent monotypic immunoglobulin. The study illustrates the need for a comprehensive array of techniques to distinguish such rare non-synthesizing and non-secretory plasmacytomas from lymphoma.
Journal of submicroscopic cytology and pathology | 1995
Kazuto Yamazaki; Brian P Eyden
Journal of submicroscopic cytology and pathology | 1994
Brian P Eyden; J Ponting; H Davies; C Bartley; E Torgersen
Journal of submicroscopic cytology and pathology | 2001
Orikasa H; Ohyama R; Tsuka N; Brian P Eyden; Kazuto Yamazaki
Journal of submicroscopic cytology and pathology | 1997
C Lugassy; Brian P Eyden; L Christensen; J P Escande
Journal of submicroscopic cytology and pathology | 1996
Kazuto Yamazaki; Brian P Eyden
Journal of submicroscopic cytology and pathology | 1997
Kazuto Yamazaki; Brian P Eyden
Journal of submicroscopic cytology and pathology | 1996
Kazuto Yamazaki; Brian P Eyden
Journal of submicroscopic cytology and pathology | 1990
Brian P Eyden; J Ferguson