Does extracellular matrix of the varicose vein wall change according to clinical stage?

Does extracellular matrix of the varicose vein wall change according to clinical stage?

The etiology and pathophysiology of chronic venous disease is not fully understood. This study aimed to determine the variation of the extracellular matrix proteins in varicose vein wall according to clinical stage. Forty varicose and 10 control veins were sampled from the saphenofemoral junction. T...

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Bibliographic Details
Published in:Ulusal cerrahi dergisi Vol. 30; no. 4; pp. 186 - 191
Main Authors: Demirkıran, Mehmet Ali, Köksoy, Cüneyt, Heper, Aylin Okçu, Bengisun, Uğur
Format: Journal Article
Language:English
Published: Turkey Turkish Journal of Surgery 2014
Subjects:
Original Investigation
Chronic venous disease
extracellular matrix proteins
varicose veins
CEAP
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Summary:The etiology and pathophysiology of chronic venous disease is not fully understood. This study aimed to determine the variation of the extracellular matrix proteins in varicose vein wall according to clinical stage. Forty varicose and 10 control veins were sampled from the saphenofemoral junction. The Clinical Etiologic Anatomic Pathophysiologic (CEAP) classification was used in patients with varicose veins. Samples were stained with hematoxylin-eosin, Masson's trichrome, EVG (Elastica-van Gieson) stain and with laminin, fibronectin, tenascin antibodies. Stained samples were examined immuno-histochemically. Changes in extracellular matrix were determined semi-quantitatively using light microscopy. It was observed that in the early stages (C2-C3) of chronic venous disease, fibrosis is increased in the intima and media layers, with fragmentation in lamina elastica interna, and increased tenascin expression in the intima layer. In advanced stages (C4-C6), the accumulation of tenascin in the intima continued along with fibrosis in the media layer, the thickness of the media layer increased and fibronectin deposition was observed. This study showed that changes first occur in the intima during the early stages of the disease with addition of alterations in the media layer at later stages.
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ISSN:1300-0705
1308-8521
DOI:10.5152/UCD.2014.2664