The urokinase receptor associated protein (uPARAP/endo180): a novel internalization receptor connected to the plasminogen activation system

Research output: Contribution to journalReviewResearchpeer-review

Standard

The urokinase receptor associated protein (uPARAP/endo180) : a novel internalization receptor connected to the plasminogen activation system. / Engelholm, L H; Nielsen, B S; Danø, K; Behrendt, N.

In: Trends in Cardiovascular Medicine, Vol. 11, No. 1, 01.2001, p. 7-13.

Research output: Contribution to journalReviewResearchpeer-review

Harvard

Engelholm, LH, Nielsen, BS, Danø, K & Behrendt, N 2001, 'The urokinase receptor associated protein (uPARAP/endo180): a novel internalization receptor connected to the plasminogen activation system', Trends in Cardiovascular Medicine, vol. 11, no. 1, pp. 7-13.

APA

Engelholm, L. H., Nielsen, B. S., Danø, K., & Behrendt, N. (2001). The urokinase receptor associated protein (uPARAP/endo180): a novel internalization receptor connected to the plasminogen activation system. Trends in Cardiovascular Medicine, 11(1), 7-13.

Vancouver

Engelholm LH, Nielsen BS, Danø K, Behrendt N. The urokinase receptor associated protein (uPARAP/endo180): a novel internalization receptor connected to the plasminogen activation system. Trends in Cardiovascular Medicine. 2001 Jan;11(1):7-13.

Author

Engelholm, L H ; Nielsen, B S ; Danø, K ; Behrendt, N. / The urokinase receptor associated protein (uPARAP/endo180) : a novel internalization receptor connected to the plasminogen activation system. In: Trends in Cardiovascular Medicine. 2001 ; Vol. 11, No. 1. pp. 7-13.

Bibtex

@article{426892be50254c34aad3bcca955e3eb9,
title = "The urokinase receptor associated protein (uPARAP/endo180): a novel internalization receptor connected to the plasminogen activation system",
abstract = "The urokinase-mediated plasminogen activation system plays a central role in the extracellular proteolytic degradation reactions in cancer invasion. In this review article we discuss a number of recent findings identifying a new cellular receptor protein, uPARAP, that interacts with components of this proteolytic system. uPARAP is a high molecular weight type-1 membrane protein, belonging to the macrophage mannose receptor protein family. On the surface of certain cells, uPARAP forms a ternary complex with the pro-form of the urokinase-type plasminogen activator (uPA) and its primary receptor (uPAR). While the biological consequences of this reaction have not yet been verified experimentally, a likely event is ligand internalization because uPARAP is a constitutively recycling internalization receptor. uPARAP also binds at least one component, collagen type V, in the extracellular matrix meshwork, pointing to a potential role in proteolytic substrate presentation. Additional ligands have been proposed, including collagenase-3 and glycoproteins capable of interacting with one of the multiple carbohydrate recognition-type domains of uPARAP. In various adult tissues uPARAP is present on fibroblasts, macrophages and a subset of endothelial cells. In fetal tissues the protein has also been demonstrated in certain bone forming regions. Hypotheses on the physiological function of uPARAP include regulatory roles in extracellular proteolysis. This type of function would be likely to direct the local turnover of proteases and their substrate degradation products and thus may add to the complicated interplay between several cell types in governing restricted tissue degradation.",
keywords = "Animals, Humans, Mannose-Binding Lectins, Membrane Glycoproteins, Neoplasms, Peptide Hydrolases, Plasminogen Activators, Protein Binding, Receptors, Cell Surface, Receptors, Urokinase Plasminogen Activator, Urokinase-Type Plasminogen Activator, Journal Article, Review",
author = "Engelholm, {L H} and Nielsen, {B S} and K Dan{\o} and N Behrendt",
year = "2001",
month = jan,
language = "English",
volume = "11",
pages = "7--13",
journal = "Trends in Cardiovascular Medicine",
issn = "1050-1738",
publisher = "Elsevier",
number = "1",

}

RIS

TY - JOUR

T1 - The urokinase receptor associated protein (uPARAP/endo180)

T2 - a novel internalization receptor connected to the plasminogen activation system

AU - Engelholm, L H

AU - Nielsen, B S

AU - Danø, K

AU - Behrendt, N

PY - 2001/1

Y1 - 2001/1

N2 - The urokinase-mediated plasminogen activation system plays a central role in the extracellular proteolytic degradation reactions in cancer invasion. In this review article we discuss a number of recent findings identifying a new cellular receptor protein, uPARAP, that interacts with components of this proteolytic system. uPARAP is a high molecular weight type-1 membrane protein, belonging to the macrophage mannose receptor protein family. On the surface of certain cells, uPARAP forms a ternary complex with the pro-form of the urokinase-type plasminogen activator (uPA) and its primary receptor (uPAR). While the biological consequences of this reaction have not yet been verified experimentally, a likely event is ligand internalization because uPARAP is a constitutively recycling internalization receptor. uPARAP also binds at least one component, collagen type V, in the extracellular matrix meshwork, pointing to a potential role in proteolytic substrate presentation. Additional ligands have been proposed, including collagenase-3 and glycoproteins capable of interacting with one of the multiple carbohydrate recognition-type domains of uPARAP. In various adult tissues uPARAP is present on fibroblasts, macrophages and a subset of endothelial cells. In fetal tissues the protein has also been demonstrated in certain bone forming regions. Hypotheses on the physiological function of uPARAP include regulatory roles in extracellular proteolysis. This type of function would be likely to direct the local turnover of proteases and their substrate degradation products and thus may add to the complicated interplay between several cell types in governing restricted tissue degradation.

AB - The urokinase-mediated plasminogen activation system plays a central role in the extracellular proteolytic degradation reactions in cancer invasion. In this review article we discuss a number of recent findings identifying a new cellular receptor protein, uPARAP, that interacts with components of this proteolytic system. uPARAP is a high molecular weight type-1 membrane protein, belonging to the macrophage mannose receptor protein family. On the surface of certain cells, uPARAP forms a ternary complex with the pro-form of the urokinase-type plasminogen activator (uPA) and its primary receptor (uPAR). While the biological consequences of this reaction have not yet been verified experimentally, a likely event is ligand internalization because uPARAP is a constitutively recycling internalization receptor. uPARAP also binds at least one component, collagen type V, in the extracellular matrix meshwork, pointing to a potential role in proteolytic substrate presentation. Additional ligands have been proposed, including collagenase-3 and glycoproteins capable of interacting with one of the multiple carbohydrate recognition-type domains of uPARAP. In various adult tissues uPARAP is present on fibroblasts, macrophages and a subset of endothelial cells. In fetal tissues the protein has also been demonstrated in certain bone forming regions. Hypotheses on the physiological function of uPARAP include regulatory roles in extracellular proteolysis. This type of function would be likely to direct the local turnover of proteases and their substrate degradation products and thus may add to the complicated interplay between several cell types in governing restricted tissue degradation.

KW - Animals

KW - Humans

KW - Mannose-Binding Lectins

KW - Membrane Glycoproteins

KW - Neoplasms

KW - Peptide Hydrolases

KW - Plasminogen Activators

KW - Protein Binding

KW - Receptors, Cell Surface

KW - Receptors, Urokinase Plasminogen Activator

KW - Urokinase-Type Plasminogen Activator

KW - Journal Article

KW - Review

M3 - Review

C2 - 11413046

VL - 11

SP - 7

EP - 13

JO - Trends in Cardiovascular Medicine

JF - Trends in Cardiovascular Medicine

SN - 1050-1738

IS - 1

ER -

ID: 180823283