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Exosomes are small cell-derived vesicles of 40-100 nm in size and are of endocytic origin. Initially, exosomes were regarded as the vehicles for the removal of unnecessary cellular proteins. Lately, exosomes are considered as important drivers of intercellular communication. Practically every cell secretes exosomes and these nanovesicles are representatives of the cell of origin. Exosomes are found in all biofluids including blood, milk, urine, sweat, tears, and culture supernatant. Explore the biology of exosomes below.
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Biogenesis
Early endosomes loaded with ubiquitinated proteins, upon recognition by ESCRT (Endosomal Sorting Complex Required for Transport), allows the formation of intraluminal vesicles (ILVs), which in turn become multivesicular bodies (MVBs), some of which are degraded in lysosomes. The fusion of MVBs with the plasma membrane causes the release of exosomes into the extracellular space.
Composition
Exosomes contain a complex composition of molecules, including proteins, lipids, microRNA, and mRNA, which are cataloged in the EXoCarta database (https://www.exocarta.org/). The most common exosomal proteins are membrane transporters and fusion proteins (Annexins, GTPases and flotillin), heat shock proteins, tetraspanins (CD9, CD63 and CD81), MVB synthesis proteins (Alix and TSG101), lipid-related proteins and phospholipases. Proteins such as CD9, CD63, CD81, TSG101, Alix and HSP70 are common to most exosomes. Exosomes are enriched with lipids like cholesterol, sphingolipids, ceramide, glycolipid GM3, and glycerophospholipids containing long, saturated fatty-acyl chains.
Mechanism of Action
Exosomes play a key role in cell-to-cell communication by merging with a recipient cell. Exosomes may remain stably associated with the plasma membrane or are internalized via an endocytic pathway, releasing their contents. The biological property of the target cell can then be altered at the genetic level (exosomal RNA), epigenetic level (exosomal miRNA) or at the protein level. Beneficial (e.g. enhancing the immune status) or detrimental (e.g. disseminating pathogenesis) outcomes are possible with these interactions. An example of a beneficial outcome is the successful suppression of the maternal immune system during pregnancy that is facilitated by exosomes. Placenta-derived exosomes exhibit immunosuppressive properties by the expression of markers such as Fas ligand (FasL), TRAIL, and PD-L1 inducing T cell death and downregulating NK activity via the expression of NKG2D ligands such as MICA/B and RAEγ1/ULBPs. Other placental exosome-associated proteins include CD247, membranous TGFβ1, placental alkaline phosphatase (PLAP), pregnancy specific glycoprotein 3, and trophoblast glycoprotein 5T4.
Characterization of Exosomes
Analysis of exosomes and their contents can reveal a lot about the host cell and also underlying pathophysiological conditions such as cancer, neurological disorders, heart disease, immunological dysregulation, and infectious disease, to name a few. Therefore, exosomes are regarded as potential biomarkers as well as therapeutic agents. Techniques such as flow cytometry, Western blotting, immunofluorescence, electron microscopy and PCR are extensively used to study both the surface proteins as well as internal exosomal contents. BioLegend provides antibodies to many surface and internal protein targets, which can be used to immunophenotype and molecularly characterize exosomes.
Markers for immune cell derived exosomes
Since exosomal contents can indicate the cell of origin, it is reasonable to predict the immune signature of a particular type of exosome. For example, exosomes derived from professional antigen-presenting cells express MHC I, MHC II, adhesion and costimulatory molecules, such as CD80 and CD86. Similarly, NK cell-derived exosomes enclose perforin and granzyme B.
BioLegend offers a comprehensive list of anti-human, mouse and rat antibodies directed towards a wide variety of protein targets (both surface and intracellular) which can help characterize exosomes via applications such as flow cytometry, Western blot, fluorescent microscopy and IHC. Refer to our cell markers page in order to find immune cell specific markers which in turn can help determine markers for exosomes originating from a particular cell type. The last tab above cites specific BioLegend products that have been used in the characterization of exosomes.
Tumor exosomal markers
The direct interaction between tumor cells and their environment plays a key role in tumor progression, for which exosomes play an important role in establishing cell-cell contact. Exosomes released into the extracellular milieu can promote angiogenesis, tumor proliferation, and thrombosis, in addition to the remodeling of the extracellular matrix. Exosomal markers for some of the common cancers are described below.
| Disease | Exosomal markers |
|---|---|
| Melanoma | CD63, CD146, Caveolin-1, TYRP1, TYRP2, VLA-4, HSP70, HSP90 |
| Glioblastoma | CD63, EGFR, Podoplanin, IDH1 (R132H mutant), EGFRVIII |
| Prostate cancer | Survivin, PSA, PCA3 |
| Bladder cancer | EGF, CD227 (Mucin-1), Gs alpha subunit, retinoic acid induced protein 3 |
| Breast cancer | CD24, CD340(erbB2/HER-2) , CD326 (EpCAM) |
| Ovarian cancer | CD44, CD171, CD24, ADAM10, CD147, claudin, CD326, MMP2 , MMP9, uPA |
| Gastric cancer | CD196 (CCR6), CD340(erbB2/HER-2), CD147 (EMMPRIN), C-MET |
| Renel cell carcinoma | CD49e, CD49f, CD105/Endoglin |
| Tumor cell proliferation | TGF-b1, FGF basic, MCP-1/CCL2, XIAP, SCF |
| Epithelial to Mesenchymal Transition (EMT) | ILK1, Caveolin-1, MMPs, Wnt-11, CD49c |
Exosomes in Neurological Disorders
Exosomes are proposed to be novel mediators in the normal development and physiology of the nervous system, playing functional roles during development and regeneration of neurons, and as mediators of cell-cell communication between neurons, oligodendrocytes, and other cells within the CNS.
On the other hand, recent research indicates that exosomes can spread “toxic” forms of mutated or misfolded proteins that are associated with neurodegenerative diseases. These include Amyloid beta, α-Synuclein, and Prion protein (PrP), which are associated with Alzheimer's disease, Parkinson's disease, and Prion disease, respectively.
BioLegend offers antibodies against a wide variety of proteins that can help characterize exosomes originating from various cell types of the CNS.
| Cell type | Exosomal markers |
|---|---|
| Neurons | Wntless (GPR177), NEDD4, NEDD4L, APP, NDFIP1, MAP1b, ITCH, Cystatin C, tau proteins, CD230 (PrP), Amyloid beta, α-Synuclein |
| Oligodendrocytes | MBP, PLP, MOG, CNPase |
| Astrocytes | Endostatin, PAR4, TIMP-1, MMP-3, MMP-9, CXCL1, CCL2, CCL3, Pentraxin 3, HSP70 |
| Microglia | Rab7, Rab11, CD107a, CD107b, CD9, CD13, CD63, MHC II |
| Citation | Pubmed | Products |
|---|---|---|
| Exosomes released from macrophages infected with intracellular pathogens stimulate a proinflammatory response in vitro and in vivo. | PubMed | Human CD63, CD81, CD86 |
| Cancer exosomes express CD39 and CD73, which suppress T cells through adenosine production. | PubMed | Human CD39, CD73 |
| Plasma-derived MHC class II+ exosomes from tumor-bearing mice suppress tumor antigen-specific immune responses. | PubMed | Mouse Alix |
| CD169 mediates the capture of exosomes in spleen and lymph node. | PubMed, Suppl. Data |
Mouse CD24 |
| Exosomes from red blood cell units bind to monocytes and induce proinflammatory cytokines, boosting T-cell responses in vitro. | PubMed | Human CD142 |
| Human B Cell-Derived Lymphoblastoid Cell Lines Constitutively Produce Fas Ligand and Secrete MHCII+FasL+ Killer Exosomes. | PubMed | Human MHC II |
| Exosomes released by islet-derived mesenchymal stem cells trigger autoimmune responses in NOD mice. | PubMed | Mouse CD63, CD81 |
| Development of glomerulus-, tubule-, and collecting duct-specific mRNA assay in human urinary exosomes and microvesicles. | PubMed | Human CD63 |
| Antigenic composition of single nano-sized extracellular blood vesicles. | PubMed | Human CD31, CD63, CD81 |
| Urinary podocyte microparticles identify prealbuminuric diabetic glomerular injury. | PubMed | Annexin V, mouse Podoplanin |
| Extracellular vesicles in urine of women with but not without kidney stones manifest patterns similar to men: a case control study. | PubMed | Human EGFR and MCP-1 |
| Lipoprotein-apheresis reduces circulating microparticles in individuals with familial hypercholesterolemia. | PubMed | Human CD11b, CD144, CD235a |
| Microvesicles released from human renal cancer stem cells stimulate angiogenesis and formation of lung premetastatic niche. | PubMed | Human CD49e, CD49f, CD105, MHC I |
| Exosomes neutralize synaptic-plasticity-disrupting activity of Aβ assemblies in vivo. | PubMed | Anti-β-Amyloid |
| A role for the eIF4E-binding protein 4E-T in P-body formation and mRNA decay. | PubMed | Anti-HA |
| Exosomes secreted by cortical neurons upon glutamatergic synapse activation specifically interact with neurons. | PubMed | Anti-GFP |
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