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Published in: Endocrine Pathology 3/2010

01-09-2010

VEGF and CD31 Association in Pituitary Adenomas

Authors: Carolina Cristina, María Inés Perez-Millan, Guillermina Luque, Raúl Ariel Dulce, Gustavo Sevlever, Silvia Inés Berner, Damasia Becu-Villalobos

Published in: Endocrine Pathology | Issue 3/2010

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Abstract

Pituitary tumors are usually less vascularized than the normal pituitary, and the role of angiogenesis in these adenomas is contentious. Appraisal of microvascular density and expression of the potent angiogenic vascular endothelial growth factor (VEGF) by immunohistochemistry has yielded controversial results, as a broad spectrum of immunostaining can be found. We determined the protein expression of VEGF and CD31, an endothelial marker, in a series of 56 surgically removed pituitary adenomas using Western blot assay. Prolactinomas had higher VEGF protein expression compared to nonfunctioning or ACTH- and GH-secreting adenomas, while CD31 was similar in the different adenoma histotypes. VEGF and CD31 were not affected by sex, age, years of adenoma evolution, or proliferation rate (Ki67 and PCNA) for all adenoma types. Only in nonfunctioning adenomas CD31 concentration increased significantly with age. There was a positive correlation between CD31 and VEGF expression when all adenoma histotypes were considered, or when prolactinomas and nonfunctioning adenomas were evaluated separately. The positive association of VEGF and CD31 expression suggests the participation of angiogenesis in adenoma development, while epithelial cell proliferation in pituitary tumors is not directly related to VEGF or CD31 expression, and other factors, such as primary genetic alterations may be involved.
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Metadata
Title
VEGF and CD31 Association in Pituitary Adenomas
Authors
Carolina Cristina
María Inés Perez-Millan
Guillermina Luque
Raúl Ariel Dulce
Gustavo Sevlever
Silvia Inés Berner
Damasia Becu-Villalobos
Publication date
01-09-2010
Publisher
Springer US
Published in
Endocrine Pathology / Issue 3/2010
Print ISSN: 1046-3976
Electronic ISSN: 1559-0097
DOI
https://doi.org/10.1007/s12022-010-9119-6

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