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Multi-omics characterization of a diet-induced obese model of non-alcoholic steatohepatitis
被引:0
|作者:
Helene M. Ægidius
Sanne S. Veidal
Michael Feigh
Philip Hallenborg
Michele Puglia
Tune H. Pers
Niels Vrang
Jacob Jelsing
Birgitte R. Kornum
Blagoy Blagoev
Kristoffer T. G. Rigbolt
机构:
[1] Gubra,
[2] Hørsholm Kongevej 11B,undefined
[3] Department of Biochemistry and Molecular Biology,undefined
[4] University of Southern Denmark,undefined
[5] Novo Nordisk Foundation Center for Basic Metabolic Research,undefined
[6] University of Copenhagen,undefined
[7] Department of Neuroscience,undefined
[8] University of Copenhagen,undefined
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摘要:
To improve the understanding of the complex biological processes underlying the development of non-alcoholic steatohepatitis (NASH), a multi-omics approach combining bulk RNA-sequencing based transcriptomics, quantitative proteomics and single-cell RNA-sequencing was used to characterize tissue biopsies from histologically validated diet-induced obese (DIO) NASH mice compared to chow-fed controls. Bulk RNA-sequencing and proteomics showed a clear distinction between phenotypes and a good correspondence between mRNA and protein level regulations, apart from specific regulatory events discovered by each technology. Transcriptomics-based gene set enrichment analysis revealed changes associated with key clinical manifestations of NASH, including impaired lipid metabolism, increased extracellular matrix formation/remodeling and pro-inflammatory responses, whereas proteomics-based gene set enrichment analysis pinpointed metabolic pathway perturbations. Integration with single-cell RNA-sequencing data identified key regulated cell types involved in development of NASH demonstrating the cellular heterogeneity and complexity of NASH pathogenesis.
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