Literature DB >> 20356925

Dendritic cell podosomes are protrusive and invade the extracellular matrix using metalloproteinase MMP-14.

Christian Gawden-Bone1, Zhongjun Zhou, Emma King, Alan Prescott, Colin Watts, John Lucocq.   

Abstract

Podosomes are spot-like actin-rich structures formed at the ventral surface of monocytic and haematopoietic cells. Podosomes degrade extracellular matrix and are proposed to be involved in cell migration. A key question is whether podosomes form protrusions similar to the invadopodia of cancer cells. We characterised podosomes of immature dendritic cells using electron microscopy combined with both conventional and novel high-resolution structured illumination light microscopy. Dendritic cell podosomes are composed of actin foci surrounded by a specialised ring region that is rich in material containing paxillin. We found that podosomes were preferential sites for protrusion into polycarbonate filters impregnated with crosslinked gelatin, degrading up to 2 micrometers of matrix in 24 hours. Podosome-associated uptake of colloidal gold-labelled gelatin matrix appeared to occur via large phagosome-like structures or narrow tubular invaginations. The motor protein myosin-II was excluded from ring or core regions but was concentrated around them and the myosin-II inhibitor Blebbistatin reduced the length of podosome protrusions. Finally, we found that degradation, protrusion and endocytosis in this system are dependent on the matrix metalloproteinase MMP-14. We propose that podosomes mediate migration of dendritic cells through tissues by means of myosin-II-dependent protrusion coupled to MMP-14-dependent degradation and endocytosis.

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Year:  2010        PMID: 20356925      PMCID: PMC2858019          DOI: 10.1242/jcs.056515

Source DB:  PubMed          Journal:  J Cell Sci        ISSN: 0021-9533            Impact factor:   5.285


  50 in total

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  54 in total

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3.  Dynamics of podosome stiffness revealed by atomic force microscopy.

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Review 4.  Signaling inputs to invadopodia and podosomes.

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Review 7.  Dissecting cell adhesion architecture using advanced imaging techniques.

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Review 10.  A new front in cell invasion: The invadopodial membrane.

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