Complementarity of SOMAscan to LC-MS/MS and RNA-seq for quantitative profiling of human embryonic and mesenchymal stem cells

Billing, Anja M.; Hamidane, Hisham Ben; Bhagwat, Aditya; Cotton, Richard; Dib, Shaima S.; Kumar, Pankaj; Hayat, Shahina; Goswami, Neha; Suhre, Karsten; Rafii, Arash; Graumann, Johannes

doi:10.1016/j.jprot.2016.08.023

Cited by 39 publications

(32 citation statements)

References 32 publications

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“…The distribution for 6903 intersecting features is depicted in Fig. 5A with average correlation of 0.5 and a mode at 0.9 demonstrating better correlation than previously published for somatic cells (0.4) (49)or differentiating cells (0.2) (48), but in line with our previous study (50). PCA analysis was performed on differentially expressed features, which display good correlation (R Ͼ 0.7 and FDR Ͻ 0.05) (Fig.…”

Section: Molecular and Cellular Proteomics 1810 1955supporting

confidence: 90%

A Systems-level Characterization of the Differentiation of Human Embryonic Stem Cells into Mesenchymal Stem Cells*[S]

Billing

Dib

Bhagwat

et al. 2019

Molecular & Cellular Proteomics

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Mesenchymal stem/stromal cells (MSCs) are self-renewing multipotent cells with regenerative, secretory and immunomodulatory capabilities that are beneficial for the treatment of various diseases. To avoid the issues that come with using tissue-derived MSCs in therapy, MSCs may be generated by the differentiation of human embryonic stems cells (hESCs) in culture. However, the changes that occur during the differentiation process have not been comprehensively characterized. Here, we combined transcriptome, proteome and phosphoproteome profiling to perform an in-depth, multi-omics study of the hESCs-to-MSCs differentiation process. Based on RNA-to-protein correlation, we determined a set of high confidence genes that are important to differentiation. Among the earliest and strongest induced proteins with extensive differential phosphorylation was AHNAK, which we hypothesized to be a defining factor in MSC biology. We observed two distinct expression waves of developmental HOX genes and an AGO2-to-AGO3 switch in gene silencing. Exploring the kinetic of noncoding ORFs during differentiation, we mapped new functions to well annotated long noncoding RNAs (CARMN, MALAT, NEAT1, LINC00152) as well as new candidates which we identified to be important to the differentiation process. Phosphoproteome analysis revealed ESC and MSC-specific phosphorylation motifs with PAK2 and RAF1 as top predicted upstream kinases in MSCs. Our data represent a rich systems-level resource on ESC-to-MSC differentiation that will be useful for the study of stem cell biology.

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Section: Molecular and Cellular Proteomics 1810 1955supporting

confidence: 90%

A Systems-level Characterization of the Differentiation of Human Embryonic Stem Cells into Mesenchymal Stem Cells*[S]

Billing

Dib

Bhagwat

et al. 2019

Molecular & Cellular Proteomics

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Section: Discussionmentioning

confidence: 99%

“…Several previous studies have validated SOMAscan using other orthogonal proteomic platforms, including LC-MS/MS and ELISA 5 – 11 . In an analysis of human embryonic and mesenchymal stem cells, Billing and colleagues considered 408 proteins measured by SOMAscan, LC-MS/MS, and RNA sequencing and reported that 60% of the SOMAscan results were validated by the other two methods, which was comparable to results obtained when comparing LC-MS/MS and RNA sequencing to each other 5 . Murota and colleagues used SOMAscan to identify 33 biomarkers associated with rheumatoid arthritis and selected five proteins to validate the results using conventional immunoassays, including electrochemiluminescence assays, ELISA, and latex turbidimetric assays 6 .…”

Section: Discussionmentioning

confidence: 99%

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Stability and reproducibility of proteomic profiles measured with an aptamer-based platform

Kim

Tworoger

Stampfer

et al. 2018

Sci Rep

113

108

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The feasibility of SOMAscan, a multiplex, high sensitivity proteomics platform, for use in studies using archived plasma samples has not yet been assessed. We quantified 1,305 proteins from plasma samples donated by 16 Nurses’ Health Study (NHS) participants, 40 NHSII participants, and 12 local volunteers. We assessed assay reproducibility using coefficients of variation (CV) from duplicate samples and intra-class correlation coefficients (ICC) and Spearman correlation coefficients (r) of samples processed (i.e., centrifuged and aliquoted into separate components) immediately, 24, and 48 hours after collection, as well as those of samples collected from the same individuals 1 year apart. CVs were <20% for 99% of proteins overall and <10% for 92% of proteins in heparin samples compared to 66% for EDTA samples. We observed ICC or Spearman r (comparing immediate vs. 24-hour delayed processing) ≥0.75 for 61% of proteins, with some variation by anticoagulant (56% for heparin and 70% for EDTA) and protein class (ranging from 49% among kinases to 83% among hormones). Within-person stability over 1 year was good (ICC or Spearman r ≥ 0.4) for 91% of proteins. These results demonstrate the feasibility of SOMAscan for analyses of archived plasma samples.

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“…However, multiplex biological assays were recently combined with MS for the identification of molecules having a biological response and biomarkers of health relevance in an effect-directed approach. For example, gene reporter assays combined with LC-HRMS for determining bioactive estrogenic and anti-estrogenic compounds in environmental water samples (Jonker et al, 2015), cell-based reporter gene assays combined with LC-MS for studying metabolites of the human histamine H4 receptor ligands (Nijmeijer et al, 2012), and a multiplatform approach for protein biomarkers discovery using SOMAscan, a multiplexed aptamer-based technique, and LC-MS (Billing et al, 2016, McArdle et al, 2016). By looking at biological response molecules it can drive future studies on the biological systems affected by exposures (Rappaport, 2012) (Dennis et al, 2016a).…”

Section: Future Perspectivesmentioning

confidence: 99%

Trends in the application of high-resolution mass spectrometry for human biomonitoring: An analytical primer to studying the environmental chemical space of the human exposome

Andra

Austin

Patel

et al. 2017

Environment International

120

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Global profiling of xenobiotics in human matrices in an untargeted mode is gaining attention for studying the environmental chemical space of the human exposome. Defined as the study of a comprehensive inclusion of environmental influences and associated biological responses, human exposome science is currently evolving out of the metabolomics science. In analogy to the latter, the development and applications of high resolution mass spectrometry (HRMS) has shown potential and promise to greatly expand our ability to capture the broad spectrum of environmental chemicals in exposome studies. HRMS can perform both untargeted and targeted analysis because of its capability of full- and/or tandem-mass spectrum acquisition at high mass accuracy with good sensitivity. The collected data from target, suspect and non-target screening can be used not only for the identification of environmental chemical contaminants in human matrices prospectively but also retrospectively. This review covers recent trends and advances in this field. We focus on advances and applications of HRMS in human biomonitoring studies, and data acquisition and mining. The acquired insights provide stepping stones to improve understanding of the human exposome by applying HRMS, and the challenges and prospects for future research.

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Complementarity of SOMAscan to LC-MS/MS and RNA-seq for quantitative profiling of human embryonic and mesenchymal stem cells

Cited by 39 publications

References 32 publications

A Systems-level Characterization of the Differentiation of Human Embryonic Stem Cells into Mesenchymal Stem Cells*[S]

A Systems-level Characterization of the Differentiation of Human Embryonic Stem Cells into Mesenchymal Stem Cells*[S]

Stability and reproducibility of proteomic profiles measured with an aptamer-based platform

Trends in the application of high-resolution mass spectrometry for human biomonitoring: An analytical primer to studying the environmental chemical space of the human exposome

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