Proteogenomic analysis reveals exosomes are more oncogenic than ectosomes

Keerthikumar, Shivakumar; Gangoda, Lahiru; Liem, Michael; Fonseka, Pamali; Atukorala, Ishara; Ozcitti, Cemil; Mechler, Ádám; Adda, Christopher G.; Ang, Ching‐Seng; Mathivanan, Suresh

doi:10.18632/oncotarget.3801

Cited by 227 publications

(218 citation statements)

References 59 publications

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“…Comparing the molecular signatures of tumor- (26)(27)(28)(29) and DC-derived (our work) medium EVs will surely provide additional specific markers. So far, we have not identified a protein that would be exclusively in medium EVs, and not also in the largest ones, which the other groups working on tumorderived EVs did not evaluate: although it would be very useful, finding a specific marker for these particular EVs may be challenging.…”

Section: Discussionmentioning

confidence: 86%

“…To obtain these results, it was necessary to combine several separation procedures and to follow a nonbiased approach, rather than a molecule-or EV subtype-targeted one. Some groups have recently performed comparative proteomic analyses of medium-sized and small EVs (with or without floatation into a gradient) from platelets (19) or tumor cells (26)(27)(28)(29). Another group has compared the expression of a few surface proteins on B lymphoma-EVs immunoprecipitated with either CD9, CD63, or CD81 (30).…”

Section: Discussionmentioning

confidence: 99%

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Proteomic comparison defines novel markers to characterize heterogeneous populations of extracellular vesicle subtypes

Kowal

Arras

Colombo

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

2,607

187

2,948

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Extracellular vesicles (EVs) have become the focus of rising interest because of their numerous functions in physiology and pathology. Cells release heterogeneous vesicles of different sizes and intracellular origins, including small EVs formed inside endosomal compartments (i.e., exosomes) and EVs of various sizes budding from the plasma membrane. Specific markers for the analysis and isolation of different EV populations are missing, imposing important limitations to understanding EV functions. Here, EVs from human dendritic cells were first separated by their sedimentation speed, and then either by their behavior upon upward floatation into iodixanol gradients or by immuno-isolation. Extensive quantitative proteomic analysis allowing comparison of the isolated populations showed that several classically used exosome markers, like major histocompatibility complex, flotillin, and heatshock 70-kDa proteins, are similarly present in all EVs. We identified proteins specifically enriched in small EVs, and define a set of five protein categories displaying different relative abundance in distinct EV populations. We demonstrate the presence of exosomal and nonexosomal subpopulations within small EVs, and propose their differential separation by immuno-isolation using either CD63, CD81, or CD9. Our work thus provides guidelines to define subtypes of EVs for future functional studies.exosomes | microvesicles | ectosomes | dendritic cells | extracellular vesicles

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Section: Discussionmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 99%

Proteomic comparison defines novel markers to characterize heterogeneous populations of extracellular vesicle subtypes

Kowal

Arras

Colombo

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

2,607

187

2,948

View full text Add to dashboard Cite

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“…The presence of integrins on exosomes has previously been reported (6,49). Exosome-associated integrins are important in cancer metastasis and preferential exosome uptake by specific cells (12).…”

Section: Discussionmentioning

confidence: 94%

“…EVs, encompassing subcategories such as exosomes, microvesicles and apoptotic bodies, constitute structures secreted from cells and are surrounded by a phospholipid bilayer membrane whose constituents may reflect their cells of origin (2,3). It has been demonstrated that the content of exosomes may be selectively incorporated (4,5), with examples of oncogenic proteins enriched in exosomes compared with their cells of origin (6). The largest of the EVs are apoptotic bodies and microvesicles, both originating from the plasma membrane (7), whereas smaller EVs, so called exosomes, are formed intracellularly by multiple invaginations of the late endocytic membrane, leading to formation of vesicle-containing endosomes called multivesicular bodies (8,9).…”

mentioning

confidence: 99%

Tracing Cellular Origin of Human Exosomes Using Multiplex Proximity Extension Assays

Larssen

Wik

Czarnewski

et al. 2017

Molecular & Cellular Proteomics

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“…Proteomics studies, however, have discovered a growing set of GPCR family proteins, including GPR179 (14), GPR155 (15), GPR100 (16), and GPRC5 family proteins (17), that are cargos of extracellular vesicles. This suggests that GPCR family proteins may also mediate intercellular communications when transported to target cells via extracellular vesicles.…”

mentioning

confidence: 99%

Adaptor Protein CD2AP and L-type Lectin LMAN2 Regulate Exosome Cargo Protein Trafficking through the Golgi Complex

Kwon

Nacke

et al. 2016

Journal of Biological Chemistry

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Edited by Thomas SöllnerExosomes, 40 -150-nm extracellular vesicles, transport biological macromolecules that mediate intercellular communications. Although exosomes are known to originate from maturation of endosomes into multivesicular endosomes (also known as multivesicular bodies) with subsequent fusion of the multivesicular endosomes with the plasma membrane, it remains unclear how cargos are selected for exosomal release. Using an inducible expression system for the exosome cargo protein GPRC5B and following its trafficking trajectory, we show here that newly synthesized GPRC5B protein accumulates in the Golgi complex prior to its release into exosomes. The L-type lectin LMAN2 (also known as VIP36) appears to be specifically required for the accumulation of GPRC5B in the Golgi complex and restriction of GPRC5B transport along the exosomal pathway. This may occur due to interference with the adaptor protein GGA1-mediated trans Golgi network-to-endosome transport of GPRC5B. The adaptor protein CD2AP-mediated internalization following cell surface delivery appears to contribute to the Golgi accumulation of GPRC5B, possibly in parallel with biosynthetic/secretory trafficking from the endoplasmic reticulum. Our data thus reveal a Golgi-traversing pathway for exosomal release of the cargo protein GPRC5B in which CD2AP facilitates the entry and LMAN2 impedes the exit of the flux, respectively.

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Proteogenomic analysis reveals exosomes are more oncogenic than ectosomes

Cited by 227 publications

References 59 publications

Proteomic comparison defines novel markers to characterize heterogeneous populations of extracellular vesicle subtypes

Proteomic comparison defines novel markers to characterize heterogeneous populations of extracellular vesicle subtypes

Tracing Cellular Origin of Human Exosomes Using Multiplex Proximity Extension Assays

Adaptor Protein CD2AP and L-type Lectin LMAN2 Regulate Exosome Cargo Protein Trafficking through the Golgi Complex

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