Tissue-factor–bearing microvesicles arise from lipid rafts and fuse with activated platelets to initiate coagulation

Conde, Ian Del; Shrimpton, Corie N.; Thiagarajan, Perumal; López, José A.

doi:10.1182/blood-2004-03-1095

Cited by 888 publications

(772 citation statements)

References 46 publications

(49 reference statements)

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“…Notably, MVs have a distinct repertoire of lipids not only compared with exosomes (our unpublished data) 41 but also to the plasma membrane of origin. Indeed, MVs are enriched in cholesterol, sphingomyelin and ceramide, and contain lipid raft elements, 28 including GM1 and GM3 gangliosides and flotillin-2. 42 Accordingly, artificial liposomes, composed of the main phospholipids of the plasma membrane, neither induce fibril solubilization nor promote Ab neurotoxicity.…”

Section: Discussionmentioning

confidence: 99%

“…This sorting mechanism may be consistent with the proposed role of lipid rafts in setting up platforms to concentrate into MVs proteins destined to secretion. 28,56 Finally, processing of Ab 1-42 to Ab 1-40 may even proceed within MVs. Indeed, previous evidence showed that neuron-derived EMVs contain some components of the gsecretase complex, 57 whereas the insulin-degrading enzyme, which proteolyzes Ab 1-42 and Ab 1-40, has been detected among cargo proteins of microglial EMVs.…”

Section: Discussionmentioning

confidence: 99%

“…MVs are shed by microglia upon ATP activation 27 and originate from lipid rafts, 28 where the ATP receptor P2X 7 is localized. 29 Shed MVs selectively accumulate various cellular components, including soluble and integral proteins, lipids and nucleic acids and their composition reflects the activation state of donor microglia.…”

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confidence: 99%

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Microglia convert aggregated amyloid-β into neurotoxic forms through the shedding of microvesicles

et al. 2013

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Alzheimer's disease (AD) is characterized by extracellular amyloid-b (Ab) deposition, which activates microglia, induces neuroinflammation and drives neurodegeneration. Recent evidence indicates that soluble pre-fibrillar Ab species, rather than insoluble fibrils, are the most toxic forms of Ab. Preventing soluble Ab formation represents, therefore, a major goal in AD. We investigated whether microvesicles (MVs) released extracellularly by reactive microglia may contribute to AD degeneration. We found that production of myeloid MVs, likely of microglial origin, is strikingly high in AD patients and in subjects with mild cognitive impairment and that AD MVs are toxic for cultured neurons. The mechanism responsible for MV neurotoxicity was defined in vitro using MVs produced by primary microglia. We demonstrated that neurotoxicity of MVs results from (i) the capability of MV lipids to promote formation of soluble Ab species from extracellular insoluble aggregates and (ii) from the presence of neurotoxic Ab forms trafficked to MVs after Ab internalization into microglia. MV neurotoxicity was neutralized by the Ab-interacting protein PrP and anti-Ab antibodies, which prevented binding to neurons of neurotoxic soluble Ab species. This study identifies microglia-derived MVs as a novel mechanism by which microglia participate in AD degeneration, and suggest new therapeutic strategies for the treatment of the disease. Cell Death and Differentiation (2014) 21, 582-593; doi:10.1038/cdd.2013.180; published online 13 December 2013Alzheimer's disease (AD) is the major cause of dementia in humans. Neuronal loss and cognitive decline occurring in AD patients are traditionally linked to the accumulation in the brain of extracellular plaques consisting of short amyloid-b (Ab) peptides of 39-42 amino acids, generated by amyloidogenic cleavage of the amyloid precursor protein. 1 Among Ab peptides, Ab 1-42 and pyroglutamate-modified Ab very rapidly aggregate and initiate the complex multistep process that leads to mature fibrils and plaque. 2,3 Although association of amyloid plaques with AD has long been assumed, Ab load does not correlate with neuronal loss 4,5 and high plaque burden does not necessarily lead to dementia in humans. 6,7 Accordingly, recent evidence clearly showed that the amyloid load reaches a plateau early after the onset of clinical symptoms in AD patients 8 and does not substantially increase in size during clinical progression. 9 These observations agree with the current view that small, soluble pre-fibrillar Ab species, rather than plaques formed by insoluble Ab fibrils, are the most toxic forms of Ab. 10 These cause synaptic dysfunction and spine loss, and correlate most closely with the severity of human AD. 5,8,11 Recent biochemical studies indicated that natural sphingolipids and gangliosides, whose metabolism has been shown to be altered in AD patients, 12 destabilize and rapidly resolubilize long Ab fibrils to neurotoxic species. 13 These studies also showed that phospholipids stabilize toxic oligomers...

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Microglia convert aggregated amyloid-β into neurotoxic forms through the shedding of microvesicles

et al. 2013

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“…We investigated whether the disruption of lipid rafts from trophozoite plasma membranes affected MV formation, as it was defined previously (Del Conde et al, 2005). To assess this effect, we treated trophozoite Results are representative of two independent experiments.…”

Section: The Origin Of Microvesicles Is Plasma Membrane and Lipid Rafmentioning

confidence: 99%

“…Different reports have shown that cholesterol should influence the lipid raft microdomains on the membrane that participate in MV formation. An interesting report by Del Conde et al (2005), demonstrated that the coagulation process is dependent of the transference of tissue factors released from monocyte-MVs to platelets. This release is dependent of lipid raft microdomains.…”

Section: Microvesicle Release Is Associated With Lipid Rafts and Mvsmentioning

confidence: 99%

Microvesicles released from Giardia intestinalis disturb host-pathogen response in vitro

Evans-Osses

Mojoli

Monguió‐Tortajada

et al. 2017

European Journal of Cell Biology

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a b s t r a c tGiardia intestinalis (G.I), is an anaerobic protozoan and the aetiological agent of giardiasis, a diarrhoea present worldwide and associated with poverty. G.I has a simple life cycle alternating between cyst and trophozoite. Cysts are transmitted orally to the stomach and transform to trophozoites in the intestine by a multifactorial process. Recently, microvesicles (MVs) have been found to be released from a wide range of eukaryotic cells. We have observed a release of MVs during the life cycle of G.I., identifying MVs from active trophozoites and from trophozoites differentiating to the cyst form. The aim of the current work was to investigate the role of MVs from G.I in the pathogenesis of giardiasis. MVs from log phase were able to increase the attachment of G. intestinalis trophozoites to Caco-2 cells. Moreover, MVs from G. intestinalis could be captured by human immature dendritic cells, resulting in increased activation and allostimulation of human dendritic cells. Lipid rafts participate in the MV biogenesis and in the attachment to Caco-2 cells. Nevertheless, proteomic analysis from two types of MVs has shown slight differences at the protein levels. An understanding of biogenesis and content of MVs derived from trophozoites might have important implications in the pathogenesis of the disease.

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Content release of extracellular vesicles in a cell‐free extract

Bonsergent

Lavieu

2019

FEBS Letters

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Extracellular vesicles (EVs) transfer molecules from donor to acceptor cells. The EV‐content delivery process within the acceptor cell is poorly characterized. We developed a new cell‐free assay to assess EV‐content release in vitro. We found that EV‐cytosolic cargoes are released from EVs when isolated vesicles are incubated with purified plasma membrane sheets at acidic pH, a characteristic of the endolysosomal environment. This process is protein dependent. Our results suggest that EV‐content delivery occurs within the endo/lysosomes of acceptor cells and is triggered by acidification. This process resembles virus content delivery and may require membrane fusion. The assay presented here will facilitate investigations into the core machinery and mechanisms underlying EV content delivery.

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Tissue-factor–bearing microvesicles arise from lipid rafts and fuse with activated platelets to initiate coagulation

Cited by 888 publications

References 46 publications

Microglia convert aggregated amyloid-β into neurotoxic forms through the shedding of microvesicles

Microglia convert aggregated amyloid-β into neurotoxic forms through the shedding of microvesicles

Microvesicles released from Giardia intestinalis disturb host-pathogen response in vitro

Content release of extracellular vesicles in a cell‐free extract

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