4.6 Article

Comparison of serum and plasma as a source of blood extracellular vesicles: Increased levels of platelet-derived particles in serum extracellular vesicle fractions alter content profiles from plasma extracellular vesicle fractions

期刊

PLOS ONE
卷 17, 期 6, 页码 -

出版社

PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0270634

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资金

  1. Japan Society for the Promotion of Science (JSPS), Japan [18H02585, 16H05325]
  2. Precursory Research for Embryonic Science and Technology (PRESTO) of the Japan Science and Technology Agency (JST) [JPMJPR17H8]
  3. Japan Agency for Medical Research and Development [JP18dk0207030, JP21dk0207042]
  4. Human Frontier Science Program [RGY0066/2017]
  5. Uehara Memorial Foundation
  6. Nakatani Foundation
  7. Tokyo Biochemical Research Foundation
  8. Asahi Glass Foundation
  9. Mochida Memorial Foundation
  10. Nakatomi Foundation

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This study comprehensively characterized EV fractions derived from plasma and serum, and found that serum EVs contain more particles and enriched platelet-associated proteins compared to plasma EVs. Therefore, the choice of plasma or serum as a source of blood EVs may qualitatively and quantitatively alter the characteristics of EVs.
Extracellular vesicles (EVs) have attracted much attention as potential diagnostic biomarkers for human diseases. Although both plasma and serum are utilized as a source of blood EVs, it remains unclear whether, how and to what extent the choice of plasma and serum affects the experimental results. To address this issue, in this study, we performed comprehensive characterization of EV fractions derived from plasma and serum, and investigated the differences between these blood EVs. We demonstrated by nanoparticle tracking analysis that EV fractions derived from serum contain more particles than those from plasma of mice. Proteomic analysis demonstrated that platelet-associated proteins are selectively enriched in serum EV fractions from both mice and humans. A literature review of proteomic data of human blood EVs reported by other groups further confirmed that selective enrichment of platelet-associated proteins is commonly observed in serum EVs, and confers different proteome profiles to plasma EVs. Our data provide experimental evidence that EV fractions derived from serum generally contain additional EVs that are released from platelets, which may qualitatively and quantitatively alter EV profiles when using serum as a source of blood EVs.

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