Gene coexpression network analysis identified potential biomarkers in gestational diabetes mellitus progression

Zhao, Xuefei; Li, Wen

doi:10.1002/mgg3.515

Cited by 12 publications

(6 citation statements)

References 41 publications

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“…AURKB promotes survival of cancer cells by cell cycle progression with phosphorylating a series of downstream substrates, including RacGAP1 . A study of gene coexpression network analysis identified that AURKB might be valuable biomarkers of gestational diabetes mellitus (Zhao and Li, 2019). Our results of the network pharmacology analysis also revealed that AURKB was targeted by eight components in SKP and interacted with many other proteins.…”

Section: Discussionsupporting

confidence: 58%

Effects of Shenkang Pills on Early-Stage Diabetic Nephropathy in db/db Mice via Inhibiting AURKB/RacGAP1/RhoA Signaling Pathway

et al. 2022

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Diabetic nephropathy (DN) is the leading cause of end-stage renal disease, so there is an urgent need to suppress its development at early stage. Shenkang pills (SKP) are a hospital prescription selected and optimized from effective traditional Chinese medicinal formulas for clinical treatment of DN. In the present study, liquid chromatography-quadrupole-time of flight-mass spectrometry (LC-Q-TOF-MS) and total contents qualification were applied to generate a quality control standard of SKP. For verifying the therapeutic effects of SKP, db/db mice were administered intragastrically with SKP at a human-equivalent dose (1.82 g/kg) for 4 weeks. Moreover, the underlying mechanism of SKP were analyzed by the renal RNA sequencing and network pharmacology. LC-Q-TOF-MS identified 46 compounds in SKP. The total polysaccharide and organic acid content in SKP were 4.60 and 0.11 mg/ml, respectively, while the total flavonoid, saponin, and protein content were 0.25, 0.31, and 0.42 mg/ml, respectively. Treatment of SKP significantly reduced fasting blood glucose, improved renal function, and ameliorated glomerulosclerosis and focal foot processes effacement in db/db mice. In addition, SKP protected podocytes from injury by increasing nephrin and podocin expression. Furthermore, transcriptome analyses revealed that 430 and 288 genes were up and down-regulated in mice treated with SKP, relative to untreated controls. Gene ontology enrichment analysis revealed that the differentially expressed genes mainly involved in modulation of cell division and chromosome segregation. Weighted gene co-expression network analysis and network pharmacology analysis indicated that aurora kinase B (AURKB), Rac GTPase activating protein 1 (RacGAP1) and SHC binding, and spindle associated 1 (shcbp1) might be the core targets of SKP. This protein and Ras homolog family member A (RhoA) were found overexpression in db/db mice, but significantly decreased with SKP treatment. We conclude that SKP can effectively treat early-stage DN and improve renal podocyte dysfunction. The mechanism may involve down-regulation of the AURKB/RacGAP1/RhoA pathway.

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Section: Discussionsupporting

confidence: 58%

Effects of Shenkang Pills on Early-Stage Diabetic Nephropathy in db/db Mice via Inhibiting AURKB/RacGAP1/RhoA Signaling Pathway

et al. 2022

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“…A study by Deyssenroth et al 26 based on 200 placenta samples observed 17 modules, while another study by Buckberry et al based on 16 samples observed 13 modules. 27 Two other studies used microarray data: 33 modules reported by Zhao et al 28 after analysis of a previously deposited dataset of 16 samples; 17 modules reported by Cox et al 29 These differences in the number of modules reported across these studies maybe driven by study considerations (sample size, platform, etc) as well as true complexity in placental gene activity. The number of modules identified in our study falls within the range reported in the literature, and the enriched pathways are consistent with what are previously reported.…”

Section: Discussionmentioning

confidence: 99%

Placental gene network modules are associated with maternal stress during pregnancy and infant temperament

Aushev

Deyssenroth

et al. 2021

The FASEB Journal

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Maternal psychosocial stress during pregnancy (MPSP) is a known contributor to maladaptive neurobehavioral development of the offspring; however, the underlying molecular mechanisms linking MPSP with childhood outcome remain largely unknown. Transcriptome-wide gene expression data were generated using RNA-seq from placenta samples collected in a multi-ethnic urban birth cohort in New York City (n = 129). Weighted gene co-expression network analysis (WGCNA) was used to characterize placental co-expression modules, which were then evaluated for their associations with MPSP and infant temperament. WGCNA revealed 16 gene coexpression modules. One module, enriched for regulation of chromosome organization/gene expression, was positively associated with MPSP and negatively associated with Regulatory Capacity (REG), a component of infant temperament. Two other modules, enriched for cotranslational protein targeting and cell cycle regulation, respectively, displayed negative associations with MPSP and positive associations with REG. A module enriched with oxidative phosphorylation/mitochondrial translation was positively associated

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“…As with hPL, the observed results may be because the proposed changes in hormone synthesis are not evident in the term placenta. Recent findings have demonstrated, via gene set enrichment analysis, that GDM placental gene expression profiles from the first and second trimesters of pregnancy had a significant upregulation of steroidogenic pathways (Zhao & Li, 2019). Additionally, elevated plasma progesterone levels have been reported during the second trimester in women who developed GDM (Ngala et al .…”

Section: Discussionmentioning

confidence: 99%

Mitochondrial dysfunction in placental trophoblast cells experiencing gestational diabetes mellitus

Fisher

Vanderpeet

Bartho

et al. 2020

The Journal of Physiology

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Key points Mitochondrial dysfunction is known to occur in diabetic phenotypes including type 1 and 2 diabetes mellitus. The incidence of gestational diabetes mellitus (GDM) is increasing and defined as the onset of a diabetic phenotype during pregnancy. The role of placental mitochondria in the aetiology of GDM remains unclear and is an emerging area of research. Differing mitochondrial morphologies within the placenta may influence the pathogenesis of the disorder. This study observed mitochondrial dysfunction in GDM placenta when assessing whole tissue. Upon further investigation into mitochondrial isolates from the cytotrophoblast and syncytiotrophoblast, mitochondrial dysfunction appears exaggerated in syncytiotrophoblast. Assessing mitochondrial populations individually enabled the determination of differences between cell lineages of the placenta and established varying levels of mitochondrial dysfunction in GDM, in some instances establishing significance in pathways previously inconclusive or confounded when assessing whole tissue. This research lays the foundation for future work into mitochondrial dysfunction in the placenta and the role it may play in the aetiology of GDM. Abstract Mitochondrial dysfunction has been associated with diabetic phenotypes, yet the involvement of placental mitochondria in gestational diabetes mellitus (GDM) remains inconclusive. This is in part complicated by the different mitochondrial subpopulations present in the two major trophoblast cell lineages of the placenta. To better elucidate the role of mitochondria in this pathology, this study examined key aspects of mitochondrial function in placentas from healthy pregnancies and those complicated by GDM in both whole tissue and isolated mitochondria. Mitochondrial content, citrate synthase activity, reactive oxygen species production and gene expression regulating metabolic, hormonal and antioxidant control was examined in placental tissue, before examining functional differences between mitochondrial isolates from cytotrophoblast (Cyto‐Mito) and syncytiotrophoblast (Syncytio‐Mito). Our study observed evidence of mitochondrial dysfunction across multiple pathways when assessing whole placental tissue from GDM pregnancies compared with healthy controls. Furthermore, by examining isolated mitochondria from the cytotrophoblast and syncytiotrophoblast cell lineages of the placenta we established that although both mitochondrial populations were dysfunctional, they were differentially impacted. These data highlight the need to consider changes in mitochondrial subpopulations at the feto‐maternal interface when studying pregnancy pathologies.

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Gene coexpression network analysis identified potential biomarkers in gestational diabetes mellitus progression

Cited by 12 publications

References 41 publications

Effects of Shenkang Pills on Early-Stage Diabetic Nephropathy in db/db Mice via Inhibiting AURKB/RacGAP1/RhoA Signaling Pathway

Effects of Shenkang Pills on Early-Stage Diabetic Nephropathy in db/db Mice via Inhibiting AURKB/RacGAP1/RhoA Signaling Pathway

Placental gene network modules are associated with maternal stress during pregnancy and infant temperament

Mitochondrial dysfunction in placental trophoblast cells experiencing gestational diabetes mellitus

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