SÉE, Violaine; FREE, Paul; CESBRON, Yann; NATIVO, Paula; SHAHEEN, Umbreen; RIGDEN, Daniel J.; SPILLER, David G.; FERNIG, David G.; WHITE, Michael R. H.; PRIOR, Ian A.; BRUST, Mathias; LOUNIS, Brahim; LEVY, Raphael

doi:10.1021/nn9006994

hal.structure.identifier	Centre for Cell imaging
dc.contributor.author	SÉE, Violaine
hal.structure.identifier	Liverpool Institute for Nanoscale Science and Technology [LINSET]
dc.contributor.author	FREE, Paul
hal.structure.identifier	Liverpool Institute for Nanoscale Science and Technology [LINSET]
dc.contributor.author	CESBRON, Yann
hal.structure.identifier	Liverpool Institute for Nanoscale Science and Technology [LINSET]
hal.structure.identifier	Physiological Laboratory
dc.contributor.author	NATIVO, Paula
hal.structure.identifier	Liverpool Institute for Nanoscale Science and Technology [LINSET]
dc.contributor.author	SHAHEEN, Umbreen
hal.structure.identifier	School of Biological Sciences
dc.contributor.author	RIGDEN, Daniel J.
hal.structure.identifier	Centre for Cell imaging
dc.contributor.author	SPILLER, David G.
hal.structure.identifier	Liverpool Institute for Nanoscale Science and Technology [LINSET]
dc.contributor.author	FERNIG, David G.
hal.structure.identifier	Centre for Cell imaging
dc.contributor.author	WHITE, Michael R. H.
hal.structure.identifier	Physiological Laboratory
dc.contributor.author	PRIOR, Ian A.
hal.structure.identifier	Liverpool Institute for Nanoscale Science and Technology [LINSET]
dc.contributor.author	BRUST, Mathias
hal.structure.identifier	Centre de physique moléculaire optique et hertzienne [CPMOH]
dc.contributor.author	LOUNIS, Brahim
hal.structure.identifier	Liverpool Institute for Nanoscale Science and Technology [LINSET]
dc.contributor.author	LEVY, Raphael
dc.date.created	2009-06-29
dc.date.issued	2009-09-22
dc.identifier.issn	1936-0851
dc.description.abstractEn	Understanding the dynamic fate and interactions of bioconjugated nanoparticles within living cells and organisms is a prerequisite for their use as in situ sensors or actuators. While recent research has provided indications on the effect of size, shape, and surface properties of nanoparticles on their internalization by living cells, the biochemical fate of the nanoparticles after internalization has been essentially unknown. Here we show that, upon internalization in a wide range of mammalian cells, biological molecules attached to the nanoparticles are degraded within the endosomal compartments through peptide cleavage by the protease cathepsin L. Importantly, using bioinformatics tools, we show that cathepsin L is able to cleave more than a third of the human proteome, indicating that this degradation process is likely to happen to most nanoparticles conjugated with peptides and proteins and cannot be ignored in the design of nanomaterials for intracellular applications. Preservation of the bioconjugates can be achieved by a combination of cathepsin inhibition and endosome disruption. Understanding the dynamic fate and interactions of bioconjugated nanoparticles within living cells and organisms is a prerequisite for their use as in situ sensors or actuators. While recent research has provided indications on the effect of size, shape, and surface properties of nanoparticles on their internalization by living cells, the biochemical fate of the nanoparticles after internalization has been essentially unknown. Here we show that, upon internalization in a wide range of mammalian cells, biological molecules attached to the nanoparticles are degraded within the endosomal compartments through peptide cleavage by the protease cathepsin L. Importantly, using bioinformatics tools, we show that cathepsin L is able to cleave more than a third of the human proteome, indicating that this degradation process is likely to happen to most nanoparticles conjugated with peptides and proteins and cannot be ignored in the design of nanomaterials for intracellular applications. Preservation of the bioconjugates can be achieved by a combination of cathepsin inhibition and endosome disruption.
dc.language.iso	en
dc.publisher	American Chemical Society
dc.subject.en	peptide
dc.subject.en	self-assembled monolayer
dc.subject.en	endocytosis
dc.subject.en	bionanotechnology
dc.subject.en	nanomedicine
dc.subject.en	gold nanoparticles
dc.subject.en	protease
dc.title.en	Cathepsin L Digestion of Nanobioconjugates upon Endocytosis
dc.type	Article de revue
dc.identifier.doi	10.1021/nn9006994
bordeaux.journal	ACS Nano
bordeaux.page	2461-8
bordeaux.volume	3
bordeaux.issue	9
bordeaux.peerReviewed	oui
hal.identifier	hal-00670490
hal.version	1
hal.popular	non
hal.audience	Internationale
hal.origin.link	https://hal.archives-ouvertes.fr//hal-00670490v1
bordeaux.COinS	ctx_ver=Z39.88-2004&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.jtitle=ACS%20Nano&rft.date=2009-09-22&rft.volume=3&rft.issue=9&rft.spage=2461-8&rft.epage=2461-8&rft.eissn=1936-0851&rft.issn=1936-0851&rft.au=S%C3%89E,%20Violaine&FREE,%20Paul&CESBRON,%20Yann&NATIVO,%20Paula&SHAHEEN,%20Umbreen&rft.genre=article

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