Extracellular proteolysis in macrophage migration: Losing grip for a breakthrough

Vérollet, Christel; Charrière, Guillaume M.; Labrousse, Arnaud; Cougoule, Céline; Cabec, Véronique Le; Maridonneau‐Parini, Isabelle

doi:10.1002/eji.201141538

Cited by 82 publications

(67 citation statements)

References 92 publications

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“…5A). Consistent with previous reports (Van Goethem et al, 2010;Vérollet et al, 2011), we found formation of elongated protrusions, which showed F-actin enrichment at their tips. Strikingly, the tips were also enriched in MT1-MMP-mCherry, pointing to a potential degradative capacity of these structures (Fig.…”

Section: Introductionsupporting

confidence: 82%

“…Within tissues, however, cells are surrounded by a three-dimensional environment, which is expected to influence both regulatory pathways involved in matrix degradation as well as the matrix-degrading organelles themselves. Indeed, primary human macrophages in gelled collagen I matrix have been shown to form long, dynamic protrusions that enriched are at their tips in podosome components such as F-actin, cortactin, talin, vinculin and CD44 (Van Goethem et al, 2010;Vérollet et al, 2011). Colocalisation of these structures with matrix defects and also with fluorescence signals in the collagen dequenching assay support the idea that these structures exhibit degradative capacity (Van Goethem et al, 2010).…”

Section: Discussionmentioning

confidence: 97%

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A specific subset of RabGTPases controls cell surface exposure of MT1-MMP, extracellular matrix degradation and 3D invasion of macrophages

Wiesner

Azzouzi

Linder

2013

Journal of Cell Science

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SummaryThe matrix metalloproteinase MT1-MMP has a major impact on invasive cell migration in both physiological and pathological settings such as immune cell extravasation or metastasis of cancer cells. Surface-associated MT1-MMP is able to cleave components of the extracellular matrix, which is a prerequisite for proteolytic invasive migration. However, current knowledge on the molecular mechanisms that regulate MT1-MMP trafficking to and from the cell surface is limited. We have identified three members of the RabGTPase family, Rab5a, Rab8a and Rab14, as crucial regulators of MT1-MMP trafficking and function in primary human macrophages. Both overexpressed and endogenous forms show prominent colocalisation with MT1-MMP-positive vesicles, whereas expression of mutant constructs, as well as siRNA-induced knockdown, reveal that these RabGTPases are crucial in the regulation of MT1-MMP surface exposure, contact of MT1-MMP-positive vesicles with podosomes, extracellular matrix degradation in two and three dimensions, as well as three-dimensional proteolytic invasion of macrophages. Collectively, our results identify Rab5a, Rab8a and Rab14 as major regulators of MT1-MMP trafficking and invasive migration of primary human macrophages, which could be promising potential targets for manipulation of immune cell invasion.

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Section: Introductionsupporting

confidence: 82%

Section: Discussionmentioning

confidence: 97%

A specific subset of RabGTPases controls cell surface exposure of MT1-MMP, extracellular matrix degradation and 3D invasion of macrophages

Wiesner

Azzouzi

Linder

2013

Journal of Cell Science

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“…TMJ disk displacement induces progressive degradation of connective tissue ECM and histopathological changes that eventually lead to permanent loss of function (Vérollet et al, 2011). Normal TMJ disk contains ECM macromolecules, i.e.…”

Section: Discussionmentioning

confidence: 99%

ADAM10 localization in temporomandibular joint disk with internal derangement: an ex vivo immunohistochemical study

et al. 2016

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Abstract:The purpose of this study was to determine the presence of ADAM10 in temporomandibular joint disk with internal derangement. Twentyfive paraffin blocks of displaced temporomandibular joint (TMJ) disk specimens from earlier investigations were retrieved from the archives of the University of Catania. Of these 16 had been removed from females and 9 from males; 11 with anterior disk displacement with reduction (ADDwR) and 14 with anterior disk displacement without reduction (ADDwoR). The sections were dehydrated, embedded in paraffin and cut. Then they were incubated in 0.3% H2O2/methanol and half of sections from each sample were incubated in diluted rabbit polyclonal anti-ADAM10 antibody. Then biotinylated antimouse/anti-rabbit IgG was applied to the sections, followed by avidin-biotinperioxidase complex. The results were analyzed and the results were that ADAM10 was overexpressed in the posterior band of sections from patients with ADDwR compared to the other bands of both ADDwR and ADDwoR sections. Overexpression correlated with severe histopathological degeneration. We believe these results have the potential to provide insights into the pathogenesis of TMJ disk degeneration and to help design new therapeutic approaches targeting the proteolytic events that lead to tissue degeneration. Early therapeutic block of ADAM10 activity could succeed in limiting aggrecan-rich matrix breakdown without affecting normal physiology.

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“…Migration in 3D dense matrices such as Matrigel requires ECM degradation for macrophages to create paths. 9 In these environments, macrophages form cell protrusions called 3D podosomes at the tip of which podosome proteins accumulate along with F-actin and matrix proteolytic activity.…”

mentioning

confidence: 99%

Podosomes are disrupted in PAPA syndrome

Maridonneau‐Parini

2014

Blood

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Extracellular proteolysis in macrophage migration: Losing grip for a breakthrough

Cited by 82 publications

References 92 publications

A specific subset of RabGTPases controls cell surface exposure of MT1-MMP, extracellular matrix degradation and 3D invasion of macrophages

A specific subset of RabGTPases controls cell surface exposure of MT1-MMP, extracellular matrix degradation and 3D invasion of macrophages

ADAM10 localization in temporomandibular joint disk with internal derangement: an ex vivo immunohistochemical study

Podosomes are disrupted in PAPA syndrome

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