Abstract
Dysfunctional visceral adipose tissue (VAT) in obesity is associated with type 2 diabetes (DM) but underlying mechanisms remain unclear. Our objective in this discovery analysis was to identify genes and proteins regulated by DM to elucidate aberrant cellular metabolic and signaling mediators. We performed label-free proteomics and RNA-sequencing analysis of VAT from female bariatric surgery subjects with DM and without DM (NDM). We quantified 1965 protein groups, 23 proteins, and 372 genes that were differently abundant in DM vs. NDM VAT. Proteins downregulated in DM were related to fatty acid synthesis and mitochondrial function (fatty acid synthase, FASN; dihydrolipoyl dehydrogenase, mitochondrial, E3 component, DLD; succinate dehydrogenase-α, SDHA) while proteins upregulated in DM were associated with innate immunity and transcriptional regulation (vitronectin, VTN; endothelial protein C receptor, EPCR; signal transducer and activator of transcription 5B, STAT5B). Transcriptome indicated defects in innate inflammation, lipid metabolism, and extracellular matrix (ECM) function, and components of complement classical and alternative cascades. The VAT proteome and transcriptome shared 13 biological processes impacted by DM, related to complement activation, cell proliferation and migration, ECM organization, lipid metabolism, and gluconeogenesis. Our data revealed a marked effect of DM in downregulating FASN. We also demonstrate enrichment of complement factor B (CFB), coagulation factor XIII A chain (F13A1), thrombospondin 1 (THBS1), and integrins at mRNA and protein levels, albeit with lower q-values and lack of Western blot or PCR confirmation. Our findings suggest putative mechanisms of VAT dysfunction in DM.
Highlights
Dysfunctional visceral adipose tissue (VAT) in obesity is associated with type 2 diabetes (DM) but underlying mechanisms remain unclear
To identify metabolic and signaling disruptions in adipose tissue associated with diabetes mellitus (DM), we conducted proteomic analysis of human Visceral adipose tissue (VAT) from 10 NDM and 10 DM age- and BMI-matched female patients with obesity. 2640 proteins were identified in total, of which 1965 had sufficient data for quantitative analysis, defined as being quantified in at least 4 samples in each group (Supplementary Tables S1, S2)
We demonstrate DM-specific VAT proteomic and transcriptomic profiles characterized by increased activity of pathways associated with inflammatory and humoral immune responses, complement activation, and cytoskeletal organization, and decreased mitochondrial function and lipid metabolic processes
Summary
Dysfunctional visceral adipose tissue (VAT) in obesity is associated with type 2 diabetes (DM) but underlying mechanisms remain unclear. Our objective in this discovery analysis was to identify genes and proteins regulated by DM to elucidate aberrant cellular metabolic and signaling mediators. The VAT proteome and transcriptome shared 13 biological processes impacted by DM, related to complement activation, cell proliferation and migration, ECM organization, lipid metabolism, and gluconeogenesis. Dysfunctional VAT in DM is characterized by adipocyte hypertrophy and cellular insulin resistance, changes in extracellular matrix (ECM) composition and function, and increased infiltration of inflammatory immune cells[3,4,5]. VAT is a key target organ in which novel molecules and pathways linked to DM pathogenesis can be identified
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