4.6 Article

SERPINE1 expression discriminates site-specific metastasis in human melanoma

期刊

EXPERIMENTAL DERMATOLOGY
卷 21, 期 7, 页码 551-554

出版社

WILEY
DOI: 10.1111/j.1600-0625.2012.01523.x

关键词

dermatopathology; melanoma; metastasis; PAI-1; SERPINE1

资金

  1. NIGMS NIH HHS [R01 GM057242, GM57242] Funding Source: Medline

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Depth of invasion, a quantifier of vertical growth, is a major cutaneous melanoma staging factor. Stromal penetrance requires pericellular proteolysis regulated by the serine protease and matrix metalloproteinase cascades. The serine protease inhibitor SERPINE1, a poor prognosis biomarker in various cancers, promotes tumor progression likely by titrating the extent and local of plasmin-initiated matrix remodelling. SERPINE1 in human melanoma was assessed using tissue arrays that included primary/metastatic tumors and normal skin. SERPINE1 was basal layer-restricted in the normal epidermis. SERPINE1 immunoreactivity was evident in 27/28 primary (96%) and 24/26 metastatic tumors (92%); cutaneous metastases (80%) had significantly elevated SERPINE1 levels compared with low signals characteristic of lymph node lesions. Moderate SERPINE1 expression was a general finding in primary melanoma, whereas reduced or increased SERPINE1 immunolocalization typified metastatic deposits. The amplitude of SERPINE1 expression may impact melanoma site-specific dissemination, with cutaneous metastases representing a high-SERPINE1 tumor subtype.

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