Abnormal Peripheral Neutrophil Transcriptome in Newly Diagnosed Type 2 Diabetes Patients

Lin, Qiuqiu; Zhou, Wenbin; Wang, Yanfei; Hao, Juan; Hui, Xiaoyan; Zhang, Zhou; Xiao, Yang

doi:10.1155/2020/9519072

Cited by 14 publications

(14 citation statements)

References 36 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In general, T2D neutrophils tended to have a stronger response to RvE1 treatment, particularly at higher, clinically relevant, RvE1 doses (Figure 3). Without any RvE1 treatment, we observed higher levels of pro-in ammatory cytokines P-Selectin and TNF-α among T2D compared to healthy neutrophils, consistent with recent evidence for enriched cytokine expression in T2D neutrophils (44), though levels of pro-in ammatory MIP-1β, IL-8, and sICAM-1 cytokines were decreased in T2D neutrophils (Figure 4). As cytokines have complex and often overlapping roles in proand anti-in ammatory pathways, the relative contribution of each cytokine to neutrophil dysfunction in T2D will require further investigation.…”

Section: Discussionsupporting

confidence: 90%

Transcriptomics of Type 2 Diabetic and Healthy Human Neutrophils

Kleinstein

McCorrison

Ahmed³

et al. 2020

Preprint

View full text Add to dashboard Cite

Objectives: Chronic inflammatory diseases, including diabetes and cardiovascular disease, are heterogeneous and often co-morbid, with increasing global prevalence. Uncontrolled type 2 diabetes (T2D) can result in severe inflammatory complications. As neutrophils are essential to inflammation, we conducted RNA-seq transcriptomic analyses to investigate the association between neutrophil gene expression and T2D phenotype. Further, as specialized pro-resolving lipid mediators, including resolvin E1 (RvE1), can actively resolve inflammation, we further surveyed the impact of RvE1 on isolated neutrophils. Methods: Cell isolation and RNA-seq analysis of neutrophils from N=11 T2D and N=7 healthy individuals with available clinical data was conducted. Additionally, cultured neutrophils (N=3 T2D, N=3 healthy) were perturbed with increasing RvE1 doses (0nM, 1nM, 10nM, or 100nM) prior to RNA-seq. Data was evaluated through a bioinformatics pipeline including pathway analysis and post hoc false-discovery rate (FDR)-correction. Results: We observed significant differential expression of 50 genes between T2D and healthy neutrophils (p<0.05), including decreased T2D gene expression in inflammatory- and lipid-related genes SLC9A4, NECTIN2 and PLPP3 (p<0.003). RvE1 treatment induced dose-dependent differential gene expression (uncorrected p<0.05) across groups, including 59 healthy and 216 T2D neutrophil genes. Comparing T2D to healthy neutrophils, 1097 genes were differentially expressed across RvE1 doses, including two significant genes, LILRB5 and AKR1C1 , involved in inflammation (p<0.05). Conclusions: Inflammatory- and lipid-related genes were differentially expressed between T2D and healthy neutrophils, and RvE1 dose-dependently modified gene expression in both groups. Unraveling the mechanisms regulating abnormalities in diabetic neutrophil responses could lead to better diagnostics and therapeutics targeting inflammation and inflammation resolution.

show abstract

Section: Discussionsupporting

confidence: 90%

Transcriptomics of Type 2 Diabetic and Healthy Human Neutrophils

Kleinstein

McCorrison

Ahmed³

et al. 2020

Preprint

View full text Add to dashboard Cite

show abstract

“…3 ). Without any RvE1 treatment, we observed higher levels of pro-inflammatory cytokines P-Selectin and TNF-α among T2D compared to healthy neutrophils, consistent with recent evidence for enriched cytokine expression in T2D neutrophils [ 44 ], though levels of pro-inflammatory MIP-1β, IL-8, and sICAM-1 cytokines were decreased in T2D neutrophils (Fig. 4 ).…”

Section: Discussionsupporting

confidence: 89%

“…Further, a recent study in adipose tissue showed that apolipoprotein M expression was decreased in T2D and obese individuals compared to lean individuals [ 43 ], further indicating a role for downregulation of genes in diabetes pathogenesis. A recent study investigating neutrophil gene expression in a small number of newly diagnosed diabetics compared to controls also observed neutrophil dysregulation, with > 15% of neutrophil genes differentially expressed in recently diagnosed T2D, ~ 60% of which were upregulated [ 44 ]. These vast differences in gene expression may be explained by neutrophil heterogeneity in a small number of samples, failure to fully exclude monocytes, or differences in neutrophil gene expression at onset of T2D compared to established disease.…”

Section: Discussionmentioning

confidence: 99%

Transcriptomics of type 2 diabetic and healthy human neutrophils

et al. 2021

View full text Add to dashboard Cite

Objectives Chronic inflammatory diseases, including diabetes and cardiovascular disease, are heterogeneous and often co-morbid, with increasing global prevalence. Uncontrolled type 2 diabetes (T2D) can result in severe inflammatory complications. As neutrophils are essential to normal and aberrant inflammation, we conducted RNA-seq transcriptomic analyses to investigate the association between neutrophil gene expression and T2D phenotype. As specialized pro-resolving lipid mediators (SPM) act to resolve inflammation, we further surveyed the impact of neutrophil receptor binding SPM resolvin E1 (RvE1) on isolated diabetic and healthy neutrophils. Methods Cell isolation and RNA-seq analysis of neutrophils from N = 11 T2D and N = 7 healthy individuals with available clinical data was conducted. Additionally, cultured neutrophils (N = 3 T2D, N = 3 healthy) were perturbed with increasing RvE1 doses (0 nM, 1 nM, 10 nM, or 100 nM) prior to RNA-seq. Data was evaluated through a bioinformatics pipeline including pathway analysis and post hoc false discovery rate (FDR)-correction. Results We observed significant differential expression of 50 genes between T2D and healthy neutrophils (p < 0.05), including decreased T2D gene expression in inflammatory- and lipid-related genes SLC9A4, NECTIN2, and PLPP3 (p < 0.003). RvE1 treatment induced dose-dependent differential gene expression (uncorrected p < 0.05) across groups, including 59 healthy and 216 T2D neutrophil genes. Comparing T2D to healthy neutrophils, 1097 genes were differentially expressed across RvE1 doses, including two significant genes, LILRB5 and AKR1C1, involved in inflammation (p < 0.05). Conclusions The neutrophil transcriptomic database revealed novel chronic inflammatory- and lipid-related genes that were differentially expressed between T2D cells when compared to controls, and cells responded to RvE1 dose-dependently by gene expression changes. Unraveling the mechanisms regulating abnormalities in diabetic neutrophil responses could lead to better diagnostics and therapeutics targeting inflammation and inflammation resolution.

show abstract

“…Kaizer et al [ 15 ] also reported that type 1 DM and T2D shared pathogenic mechanisms, such as overexpression of IL1B (probably due to hyperglycemia). Moreover, Lin et al [ 16 ] performed RNA sequencing for neutrophils isolated from the blood of T2D patients and found that genes dysregulated in these patients were enriched in cytokine–cytokine receptor interactions, as well as nuclear factor kappa-light-chain-enhancer of activated B cells (NF-κB), tumor necrosis factor, cell adhesion molecule, Toll-like receptor, and chemokine signaling. In the OPTIMED study, whole transcriptome of T2D blood samples further revealed that genes with altered expression after anti-diabetic treatment with metformin were involved in the improvement of energy metabolism, the modulation of inflammation, and the inhibition of cancer progression [ 17 ].…”

Section: Introductionmentioning

confidence: 99%

Shared Blood Transcriptomic Signatures between Alzheimer’s Disease and Diabetes Mellitus

Lee

2021

Biomedicines

View full text Add to dashboard Cite

Alzheimer’s disease (AD) and diabetes mellitus (DM) are known to have a shared molecular mechanism. We aimed to identify shared blood transcriptomic signatures between AD and DM. Blood expression datasets for each disease were combined and a co-expression network was used to construct modules consisting of genes with similar expression patterns. For each module, a gene regulatory network based on gene expression and protein-protein interactions was established to identify hub genes. We selected one module, where COPS4, PSMA6, GTF2B, GTF2F2, and SSB were identified as dysregulated transcription factors that were common between AD and DM. These five genes were also differentially co-expressed in disease-related tissues, such as the brain in AD and the pancreas in DM. Our study identified gene modules that were dysregulated in both AD and DM blood samples, which may contribute to reveal common pathophysiology between two diseases.

show abstract

Abnormal Peripheral Neutrophil Transcriptome in Newly Diagnosed Type 2 Diabetes Patients

Cited by 14 publications

References 36 publications

Transcriptomics of Type 2 Diabetic and Healthy Human Neutrophils

Transcriptomics of Type 2 Diabetic and Healthy Human Neutrophils

Transcriptomics of type 2 diabetic and healthy human neutrophils

Shared Blood Transcriptomic Signatures between Alzheimer’s Disease and Diabetes Mellitus

Contact Info

Product

Resources

About