Expression of Urokinase Plasminogen Activator, Its Receptor and Type-1 Inhibitor in Malignant and Benign Prostate Tissue

Overview

Journal Int J Cancer

Specialty Oncology

Date 2004 Oct 30

PMID 15515049

Citations 21

Authors

Pernille Autzen Usher

Ole Frokjaer Thomsen

Peter Iversen

Morten Johnsen

Nils Brunner

Gunilla Hoyer-Hansen

Peter Andreasen

Keld Dano

Boye Schnack Nielsen

Affiliations

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Abstract

The plasminogen activation (PA) cascade participates in degradation of extracellular matrix during cancer invasion. We have studied the expression of urokinase-type plasminogen activator (uPA) mRNA, uPA receptor (uPAR) mRNA and immunoreactivity, and type-1 plasminogen activator inhibitor (PAI-1) mRNA and immunoreactivity in 16 prostate adenocarcinomas and 9 benign prostate hyperplasias. uPA mRNA and uPAR mRNA expression were found in 9 and 8 of the adenocarcinomas, respectively, and in 7 and 6 of the benign hyperplasias, respectively. In both malignant and benign lesions, expression of these 2 mRNAs was predominantly seen in cells identified as macrophages, which in most of the carcinomas (approximately 90%) were located in the interstitial tissue between the tumor cell islands, while in most of the benign hyperplasias they were located in the lumen of the glands and were in only a few cases (approximately 30%) found in the interstitial tissue. uPAR immunoreactivity correlated with the mRNA expression and was, in addition, found in neutrophils. PAI-1 mRNA was detected in 13 of the 16 carcinomas and in 8 of the 9 benign hyperplasias, located in scattered fibroblast-like cells in both groups, in some vascular structures and in a few macrophages located in the interstitial tissue of both malignant and benign lesions. A similar expression pattern was found for PAI-1 immunoreactivity. In 8 of the 16 carcinomas, all 3 components were present, and in several areas colocalization was observed in stromal cells in close proximity to cancer cell islands. No immunoreactivity and/or mRNA expression of uPA, uPAR or PAI-1 was observed in cancer cells or in other epithelial cells in any of the cases.

Citing Articles

The Urokinase Receptor (uPAR) as a "Trojan Horse" in Targeted Cancer Therapy: Challenges and Opportunities.

Metrangolo V, Ploug M, Engelholm L Cancers (Basel). 2021; 13(21).

PMID: 34771541 PMC: 8582577. DOI: 10.3390/cancers13215376.

PET imaging of urokinase-type plasminogen activator receptor (uPAR) in prostate cancer: current status and future perspectives.

Skovgaard D, Persson M, Kjaer A Clin Transl Imaging. 2016; 4(6):457-465.

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Distinct encounter complexes of PAI-1 with plasminogen activators and vitronectin revealed by changes in the conformation and dynamics of the reactive center loop.

Qureshi T, Goswami S, McClintock C, Ramsey M, Peterson C Protein Sci. 2015; 25(2):499-510.

PMID: 26548921 PMC: 4815334. DOI: 10.1002/pro.2841.

uPAR Expression Pattern in Patients with Urothelial Carcinoma of the Bladder--Possible Clinical Implications.

Dohn L, Pappot H, Iversen B, Illemann M, Hoyer-Hansen G, Christensen I PLoS One. 2015; 10(8):e0135824.

PMID: 26292086 PMC: 4546385. DOI: 10.1371/journal.pone.0135824.

Imaging active urokinase plasminogen activator in prostate cancer.

LeBeau A, Sevillano N, Markham K, Winter M, Murphy S, Hostetter D Cancer Res. 2015; 75(7):1225-35.

PMID: 25672980 PMC: 4383704. DOI: 10.1158/0008-5472.CAN-14-2185.