2019
DOI: 10.1177/1177625019840282
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Pathway-Based Analysis of the Liver Response to Intravenous Methylprednisolone Administration in Rats: Acute Versus Chronic Dosing

Abstract: Pharmacological time-series data, from comparative dosing studies, are critical to characterizing drug effects. Reconciling the data from multiple studies is inevitably difficult; multiple in vivo high-throughput -omics studies are necessary to capture the global and temporal effects of the drug, but these experiments, though analogous, differ in (microarray or other) platforms, time-scales, and dosing regimens and thus cannot be directly combined or compared. This investigation addresses this reconciliation i… Show more

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Cited by 7 publications
(16 citation statements)
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References 63 publications
(212 reference statements)
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“…Based on our earlier studies which determined that acute and chronic MPL exposure impact differentially liver (Acevedo et al, 2019), we hypothesize the drug to induce dosing-dependent and tissue-specific effects, as earlier transcriptomic analyses indicate (Ballard et al, 1974;Sun et al, 1999;Yao et al, 2008; et al, 2014). When comparing liver and muscle effects, we determine that acute dosing elicits comparable dynamics in liver and muscle, as exemplified in Figure 8 for the peroxisome signaling pathway for which the dominant regulatory structure is receptor-mediated.…”
Section: Resultsmentioning
confidence: 88%
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“…Based on our earlier studies which determined that acute and chronic MPL exposure impact differentially liver (Acevedo et al, 2019), we hypothesize the drug to induce dosing-dependent and tissue-specific effects, as earlier transcriptomic analyses indicate (Ballard et al, 1974;Sun et al, 1999;Yao et al, 2008; et al, 2014). When comparing liver and muscle effects, we determine that acute dosing elicits comparable dynamics in liver and muscle, as exemplified in Figure 8 for the peroxisome signaling pathway for which the dominant regulatory structure is receptor-mediated.…”
Section: Resultsmentioning
confidence: 88%
“…This statistic is the fraction of genes within a pathway for which gene profiles are available. To assess the confidence in the fractional coverage, an associated p-value (f c p-value) is determined using the 1-tail Fisher's Exact test such that the total rat genome is the set of unique rat genes in all KEGG's rat-relevant pathways (Acevedo et al, 2019). Pathways with low fractional occupancy yield inconclusive p-values as an artifact of the Fisher's Exact Test and were eliminated from the analysis.…”
Section: Mapping Transcriptomic Data To Pathwaysmentioning
confidence: 99%
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