Transcriptomics of type 2 diabetic and healthy human neutrophils

Transcriptomics of type 2 diabetic and healthy human neutrophils

Abstract 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 a...

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Main Authors: Sarah E. Kleinstein, Jamison McCorrison, Alaa Ahmed, Hatice Hasturk, Thomas E. Van Dyke, Marcelo Freire
Format: Article
Language:English
Published: BMC 2021-06-01
Series:BMC Immunology
Subjects:
Neutrophils
Diabetes
Gene regulation
Inflammation
Lipid mediators
Online Access:https://doi.org/10.1186/s12865-021-00428-6
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spelling doaj-98f4759616df4e76b350f03dd0fd25ca2021-06-20T11:50:37ZengBMCBMC Immunology1471-21722021-06-0122111610.1186/s12865-021-00428-6Transcriptomics of type 2 diabetic and healthy human neutrophilsSarah E. Kleinstein0Jamison McCorrison1Alaa Ahmed2Hatice Hasturk3Thomas E. Van Dyke4Marcelo Freire5Genomic Medicine and Infectious Diseases, J. Craig Venter InstituteGenomic Medicine and Infectious Diseases, J. Craig Venter InstituteThe Forsyth InstituteThe Forsyth InstituteThe Forsyth InstituteGenomic Medicine and Infectious Diseases, J. Craig Venter InstituteAbstract 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.https://doi.org/10.1186/s12865-021-00428-6NeutrophilsDiabetesGene regulationInflammationLipid mediators
collection DOAJ
language English
format Article
sources DOAJ
author Sarah E. Kleinstein
Jamison McCorrison
Alaa Ahmed
Hatice Hasturk
Thomas E. Van Dyke
Marcelo Freire
spellingShingle Sarah E. Kleinstein
Jamison McCorrison
Alaa Ahmed
Hatice Hasturk
Thomas E. Van Dyke
Marcelo Freire
Transcriptomics of type 2 diabetic and healthy human neutrophils
BMC Immunology
Neutrophils
Diabetes
Gene regulation
Inflammation
Lipid mediators
author_facet Sarah E. Kleinstein
Jamison McCorrison
Alaa Ahmed
Hatice Hasturk
Thomas E. Van Dyke
Marcelo Freire
author_sort Sarah E. Kleinstein
title Transcriptomics of type 2 diabetic and healthy human neutrophils
title_short Transcriptomics of type 2 diabetic and healthy human neutrophils
title_full Transcriptomics of type 2 diabetic and healthy human neutrophils
title_fullStr Transcriptomics of type 2 diabetic and healthy human neutrophils
title_full_unstemmed Transcriptomics of type 2 diabetic and healthy human neutrophils
title_sort transcriptomics of type 2 diabetic and healthy human neutrophils
publisher BMC
series BMC Immunology
issn 1471-2172
publishDate 2021-06-01
description Abstract 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.
topic Neutrophils
Diabetes
Gene regulation
Inflammation
Lipid mediators
url https://doi.org/10.1186/s12865-021-00428-6
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