A large scale mass spectrometry-based histone screening for assessing epigenetic developmental toxicity

Verhelst, Sigrid; Puyvelde, Bart Van; Willems, Sander; Daled, Simon; Cornelis, Senne; Corveleyn, Laura; Willems, Ewoud; Deforce, Dieter; Clerck, Laura De; Dhaenens, Maarten

doi:10.1038/s41598-022-05268-x

“…Based on the absolute abundances of the native modified K9[Poy]K14[Ac] and unmodified K9[Poy]K14[Poy] peptides, we calculated stoichiometry of the K14Ac in the donors’ samples as a percentage of total amount—a sum of K14 modified (acetylated, Ac) and unmodified (propionylated, Poy) fractions—of the investigated H3 peptide [ 17 ]. Although PTMs stoichiometry can be was determined using label free, relative MS approaches (eg [ 35 ]. ), we chose to calculate it based on the absolute amounts of modified and unmodified peptides determined in LC–MS/MS analysis in MRM mode using SIL standards.…”

Section: Resultsmentioning

confidence: 99%

Change of histone H3 lysine 14 acetylation stoichiometry in human monocyte derived macrophages as determined by MS-based absolute targeted quantitative proteomic approach: HIV infection and methamphetamine exposure

Macur,

Schissel,

Yu

et al. 2023

Clin Proteom

1

0

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Background Histones posttranslational modification represent an epigenetic mechanism that regulate gene expression and other cellular processes. Quantitative mass spectrometry used for the absolute quantification of such modifications provides further insight into cellular responses to extracellular insults such as infections or toxins. Methamphetamine (Meth), a drug of abuse, is affecting the overall function of the immune system. In this report, we developed, validated and applied a targeted, MS-based quantification assay to measure changes in histone H3 lysine 14 acetylation (H3K14Ac) during exposure of human primary macrophages to HIV-1 infection and/or Meth. Methods The quantification assay was developed and validated to determine H3K14Ac stoichiometry in histones that were isolated from the nuclei of control (CIC) and exposed to Meth before (CIM) or/and after (MIM) HIV-infection human monocyte-derived macrophages (hMDM) of six donors. It was based on LC–MS/MS measurement using multiple reaction monitoring (MRM) acquisition of the unmodified and acetylated form of lysine K14 of histone H3 9KSTGGKAPR17 peptides and the corresponding stable isotope labeled (SIL) heavy peptide standards of the same sequences. The histone samples were propionylated (Poy) pre- and post- trypsin digestion so that the sequences of the monitored peptides were: K[Poy]STGGK[1Ac]APR, K[Poy]STGGK[1Ac]APR-heavy, K[Poy]STGGK[Poy]APR and K[Poy]STGGK[Poy]APR-heavy. The absolute amounts of the acetylated and unmodified peptides were determined by comparing to the abundances of their SIL standards, that were added to the samples in the known concentrations, and, then used for calculation of H3K14Ac stoichiometry in CIC, CIM and MIM hMDM. Results The assay was characterized by LLOD of 0.106 fmol/µL and 0.204 fmol/µL for unmodified and acetylated H3 9KSTGGKAPR17 peptides, respectively. The LLOQ was 0.5 fmol/µL and the linear range of the assay was from 0.5 to 2500 fmol/µL. The absolute abundances of the quantified peptides varied between the donors and conditions, and so did the H3K14Ac stoichiometry. This was rather attributed to the samples nature itself, as the variability of their triplicate measurements was low. Conclusions The developed LC–MS/MS assay enabled absolute quantification of H3K14Ac in exposed to Meth HIV-infected hMDM. It can be further applied determination of this PTM stoichiometry in other studies on human primary macrophages. Graphical Abstract

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“…These potential biomarkers will be validated both in vitro and in vivo . Further optimization of MS analysis time could facilitate the analysis of patient samples in a clinical setting in the future 23 . Here we describe the functionalities available in the atlas, as an illustration of data reuse potential.…”

Section: Data Recordsmentioning

confidence: 99%

An interactive mass spectrometry atlas of histone posttranslational modifications in T-cell acute leukemia

Provez

¹

,

Puyvelde

²

,

Corveleyn

³

et al. 2022

Preprint

Self Cite

2

0

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The holistic nature of omics studies makes them ideally suited to generate hypotheses on health and disease. Sequencing-based genomics and mass spectrometry (MS)-based proteomics are linked through epigenetic regulation mechanisms. However, epigenomics is currently mainly focused on DNA methylation status using sequencing technologies, while studying histone posttranslational modifications (hPTMs) using MS is lagging, partly because reuse of raw data is impractical. Yet, targeting hPTMs using epidrugs is an established promising research avenue in cancer treatment. Therefore, we here present the most comprehensive MS-based preprocessed hPTM atlas to date, including 21 T-cell acute lymphoblastic leukemia (T-ALL) cell lines. We present the data in an intuitive and browsable single licensed Progenesis QIP project and provide all essential quality metrics, allowing users to assess the quality of the data, edit individual peptides, try novel annotation algorithms and export both peptide and protein data for downstream analyses, exemplified by the PeptidoformViz tool. This data resource sets the stage for generalizing MS-based histone analysis and provides the first reusable histone dataset for epidrug development.

show abstract

“…These potential biomarkers will be validated both in vitro and in vivo . Further optimization of MS analysis time could facilitate the analysis of patient samples in a clinical setting in the future 25 . Here we describe the functionalities available in the atlas, as an illustration of data reuse potential.…”

Section: Usage Notesmentioning

confidence: 99%

An interactive mass spectrometry atlas of histone posttranslational modifications in T-cell acute leukemia

Provez

¹

,

Puyvelde

²

,

Corveleyn

³

et al. 2022

Sci Data

Self Cite

2

0

View full text Add to dashboard Cite

The holistic nature of omics studies makes them ideally suited to generate hypotheses on health and disease. Sequencing-based genomics and mass spectrometry (MS)-based proteomics are linked through epigenetic regulation mechanisms. However, epigenomics is currently mainly focused on DNA methylation status using sequencing technologies, while studying histone posttranslational modifications (hPTMs) using MS is lagging, partly because reuse of raw data is impractical. Yet, targeting hPTMs using epidrugs is an established promising research avenue in cancer treatment. Therefore, we here present the most comprehensive MS-based preprocessed hPTM atlas to date, including 21 T-cell acute lymphoblastic leukemia (T-ALL) cell lines. We present the data in an intuitive and browsable single licensed Progenesis QIP project and provide all essential quality metrics, allowing users to assess the quality of the data, edit individual peptides, try novel annotation algorithms and export both peptide and protein data for downstream analyses, exemplified by the PeptidoformViz tool. This data resource sets the stage for generalizing MS-based histone analysis and provides the first reusable histone dataset for epidrug development.

show abstract

A large scale mass spectrometry-based histone screening for assessing epigenetic developmental toxicity

Cited by 7 publications

References 77 publications

Change of histone H3 lysine 14 acetylation stoichiometry in human monocyte derived macrophages as determined by MS-based absolute targeted quantitative proteomic approach: HIV infection and methamphetamine exposure

Change of histone H3 lysine 14 acetylation stoichiometry in human monocyte derived macrophages as determined by MS-based absolute targeted quantitative proteomic approach: HIV infection and methamphetamine exposure

An interactive mass spectrometry atlas of histone posttranslational modifications in T-cell acute leukemia

An interactive mass spectrometry atlas of histone posttranslational modifications in T-cell acute leukemia

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