Please use this identifier to cite or link to this item: http://hdl.handle.net/1822/1933

TitleNovel and classic myoepithelial/stem cell markers in metaplastic carcinomas of the breast
Author(s)Reis Filho, Jorge S.
Milanezi, Fernanda
Paredes, Joana
Silva, Paula
Pereira, Emílio M.
Maeda, Sueli A.
Carvalho, Leda V. de
Schmitt, Fernando C.
KeywordsBreast
Carcinosarcoma
Immunohistochemistry
Matrix-producing carcinoma
Metaplastic carcinoma
Myoepithelium
Spindle cell carcinoma
Issue date2003
PublisherLippincott, Williams & Wilkins
JournalApplied Immunohistochemistry & Molecular Morphology
Citation"Applied immunohistochemistry & molecular morphology". ISSN 1062-3345. 11:1 (2003) 1-8.
Abstract(s)Metaplastic carcinomas of the breast (MCBs) are unusual neoplasms characterized by an admixture of glandular epithelial components, which frequently exhibit features of squamous differentiation, and mesenchymal malignant components. Regardless of the presence of myoepithelial features in MCB, no consensus concerning their putative histogenesis has yet been achieved. Recently, novel putative myoepithelial markers have been developed, including p63, maspin, and P-cadherin. We assessed the expression of these myoepithelial markers in MCBs and compared their expression with classic myoepithelial markers. Immunohistochemistry using the streptavidin– biotin–peroxidase complex technique with antibodies raised against p63, maspin, P-cadherin, actin (clones CGA7, 1A4 and HHF35), cytokeratin 14 (Ck14), and vimentin was performed on 16 MCBs (7 matrix-producing MCBs, 6 adenosquamous MCBs, and 3 MCBs with heterologous elements). In healthy breast lobules and ducts adjacent to the tumors, myoepithelial cells showed distinctive and consistent immunoreactivity for p63, maspin, P-cadherin, actin, S-100 protein, and Ck14. Matrix- producing MCBs were positive for maspin in all cases, for p63 in 4 of 7 cases, and for P-cadherin in 4 of 7 cases. Adenosquamous MCB showed immunoreactivity for p63, maspin, and P-cadherin in 5 of 6 cases. All novel myoepithelial markers and Ck14 decorated squamous cell islands. MCBs with heterologous elements were positive for p63 in 1 case, for maspin in all 3 cases, and for P-cadherin in 2 cases. All cases showed at least one of the novel myoepithelial markers. Eleven of 16 cases were positive for actin. Eleven of 14 cases reacted with Ck14, and all cases that stained for S-100 protein (9 of 9) and vimentin (13 of 13) were also positive. Based on our findings, the balance of probabilities favors that MCBs may have a basal or myoepithelial cell histogenesis and differentiation.
TypeArticle
URIhttp://hdl.handle.net/1822/1933
DOI10.1097/00129039-200303000-00001
ISSN1062-3345
1533-4058
Peer-Reviewedyes
AccessOpen access
Appears in Collections:ICVS - Artigos em Revistas Internacionais com Referee

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