pmartRdata: pmartRdata
In pmartR/pmartRdata: Example Data for pmartR Package
pmartRdata R Documentation
pmartRdata
Description
The pmartRdata package contains example datasets compatible with the pmartR
package. These datasets include unlabeled (LC-MS/MS) and isobaric labeled
(TMT) peptide, protein, metabolites (GC-MS and NMR), lipids (both negative
and positive LC-MS ionization modes), and RNAseq. Some of the datasets were
generated as part of the same experiments, as described below.
Data types
Experiment 1 Data: Host response to virus using human cells. This experiment
includes isobaric labeled peptide data (TMT), negative and positive
ionization mode LC-MS lipidomics data, and RNAseq data. Sample names across
the different data types from this experiment have been harmonized, to allow
data integration. These data are a deidentified subset from an experiment
that has not yet been published. Samples included in this subset consist of
human cells infected with one of three virus strains.
Experiment 2 Data: Human tissue samples. This experiment includes unlabeled
peptide data (LC-MS/MS), the associated protein data, and metabolomics data
(GC-MS). Sample names across the different data types from this experiment
have been harmonized, to allow data integration. Note that the These data are
a deidentified subset from an experiment that has not yet been published.
Samples included in this subset consist of tissue samples from humans
exhibiting three primary phenotypes.
NMR Data: Tomato plant samples. These data are publicly available via Biais
et al. (reference listed below). Samples in this experiment each come from
one of four different time points.
Technical Replicates Peptide Data: Mouse plasma samples. These data are a
subset of the data used in Webb-Robertson et al. (reference listed below) and
include biological samples associated with one of two levels of a factor, a
dilution level of mouse plasma to Shewanella Oneidensis MR-1, and a technical
replicate (two technical replicates per biological sample).
Data formats
Each type of data is provided in two formats. The first format is an S3
object class used by the R package pmartR. Data available as S3
objects 'pepData', 'proData', 'metabData', 'lipidData', ‘nmrData’, and
‘seqData’ are created by as.pepData,
as.proData, as.metabData,
as.lipidData, as.nmrData,
as.seqData, respectively. The second format
corresponds to the individual components of the S3 object classes,
e_data - biomolecule expression data, f_data – sample meta
information, and e_meta – biomolecule expression meta data. See
pmartR for more details.
References
Webb-Robertson BJ, Matzke MM, Datta S, Payne SH, Kang J, Bramer
LM, Nicora CD, Shukla AK, Metz TO, Rodland KD, Smith RD, Tardiff MF,
McDermott JE, Pounds JG, Waters KM (2014), Bayesian proteoform
modeling improves protein quantification of global proteomic measurements.
Molecular & Cellular Proteomics. doi: 10.1074/mcp.M113.030932.
Biais B, Benard C, Beauvoit B, Colombie S, Prodhomme D, Menard G,
Bernillon S, Gehl B, Gautier H, Ballias P, et al. (2014), Remarkable
reproducibility of enzyme activity profiles in tomato fruits grown under
contrasting environments provides a roadmap for studies of fruit metabolism.
Plant Physiol 164 (3), 1204-1221. doi: 10.1104/pp.113.231241.
See Also
as.lipidData
as.metabData
as.nmrData
as.pepData
as.proData
as.seqData
pmartR/pmartRdata documentation built on Jan. 13, 2023, 3:52 a.m.
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| pmartRdata | R Documentation |
pmartRdata
Description
The pmartRdata package contains example datasets compatible with the pmartR package. These datasets include unlabeled (LC-MS/MS) and isobaric labeled (TMT) peptide, protein, metabolites (GC-MS and NMR), lipids (both negative and positive LC-MS ionization modes), and RNAseq. Some of the datasets were generated as part of the same experiments, as described below.
Data types
Experiment 1 Data: Host response to virus using human cells. This experiment includes isobaric labeled peptide data (TMT), negative and positive ionization mode LC-MS lipidomics data, and RNAseq data. Sample names across the different data types from this experiment have been harmonized, to allow data integration. These data are a deidentified subset from an experiment that has not yet been published. Samples included in this subset consist of human cells infected with one of three virus strains.
Experiment 2 Data: Human tissue samples. This experiment includes unlabeled peptide data (LC-MS/MS), the associated protein data, and metabolomics data (GC-MS). Sample names across the different data types from this experiment have been harmonized, to allow data integration. Note that the These data are a deidentified subset from an experiment that has not yet been published. Samples included in this subset consist of tissue samples from humans exhibiting three primary phenotypes.
NMR Data: Tomato plant samples. These data are publicly available via Biais et al. (reference listed below). Samples in this experiment each come from one of four different time points.
Technical Replicates Peptide Data: Mouse plasma samples. These data are a subset of the data used in Webb-Robertson et al. (reference listed below) and include biological samples associated with one of two levels of a factor, a dilution level of mouse plasma to Shewanella Oneidensis MR-1, and a technical replicate (two technical replicates per biological sample).
Data formats
Each type of data is provided in two formats. The first format is an S3
object class used by the R package pmartR. Data available as S3
objects 'pepData', 'proData', 'metabData', 'lipidData', ‘nmrData’, and
‘seqData’ are created by as.pepData,
as.proData, as.metabData,
as.lipidData, as.nmrData,
as.seqData, respectively. The second format
corresponds to the individual components of the S3 object classes,
e_data - biomolecule expression data, f_data – sample meta
information, and e_meta – biomolecule expression meta data. See
pmartR for more details.
References
Webb-Robertson BJ, Matzke MM, Datta S, Payne SH, Kang J, Bramer LM, Nicora CD, Shukla AK, Metz TO, Rodland KD, Smith RD, Tardiff MF, McDermott JE, Pounds JG, Waters KM (2014), Bayesian proteoform modeling improves protein quantification of global proteomic measurements. Molecular & Cellular Proteomics. doi: 10.1074/mcp.M113.030932.
Biais B, Benard C, Beauvoit B, Colombie S, Prodhomme D, Menard G, Bernillon S, Gehl B, Gautier H, Ballias P, et al. (2014), Remarkable reproducibility of enzyme activity profiles in tomato fruits grown under contrasting environments provides a roadmap for studies of fruit metabolism. Plant Physiol 164 (3), 1204-1221. doi: 10.1104/pp.113.231241.
See Also
as.lipidData
as.metabData
as.nmrData
as.pepData
as.proData
as.seqData
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