T Cell Histone GlcNAcylation Participates in the Epigenetics of Lupus

T 细胞组蛋白 GlcNAc 酰化参与狼疮的表观遗传学

• 批准号: 9114496
• 负责人: Gabriela Judith Gorelik
• 金额: $ 2.42万
• 依托单位: UNIVERSITY OF MICHIGAN AT ANN ARBOR
• 依托单位国家: 美国
• 财政年份: 2015
• 资助国家: 美国
• 起止时间: 2015-08-01 至 2017-01-17
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/9114496
• 关键词: Adverse effects; Affect; Americas; Autoimmune Diseases; Autoimmune Process; Autoimmunity; B-Lymphocytes; Binding; Biological; Biological Markers; CD4 Positive T Lymphocytes; Cell physiology; Cells; ChIP-seq; Chromatin; Chromatin Structure; Chronic; Complex; Coupled; DNA; DNA Methylation; DNA Sequence; Development; Diabetes Mellitus; Disease; Environmental Risk Factor; Enzymes; Epigenetic Process; Female; Foundations; Functional disorder; Future; Gene Expression; Gene Expression Regulation; Gene-Modified; Genes; Genetic; Genetic Transcription; Glucosamine; Health; Histone Code; Histones; Human; Immune; Immune response; Immunosuppression; Immunosuppressive Agents; In Vitro; Infection; Inflammatory; Link; Lupus; Mass Spectrum Analysis; MicroRNAs; Modification; Molecular; Molecular Target; Pathogenesis; Pathway interactions; Patients; Pharmaceutical Preparations; Phosphorylation; Physical condensation; Play; Post-Translational Protein Processing; Predisposition; Prevalence; Proteins; Proteomics; Quality of life; Recruitment Activity; Recurrence; Regulation; Risk; Role; Serine; Signal Pathway; Signal Transduction; Site; Substrate Specificity; Susceptibility Gene; Systemic Lupus Erythematosus; T-Lymphocyte; TNFSF5 gene; Testing; Threonine; Time; Transcriptional Activation; UDP-N-acetylglucosamine-peptide beta-N-acetylglucosaminyltransferase; Ubiquitination; United States; Woman; Work; X Chromosome; base; chromatin immunoprecipitation; chromatin remodeling; chronic autoimmune disease; demethylation; density; epigenome; gene repression; genetic approach; glycosylation; histone modification; improved; in vivo; insight; male; men; mortality; overexpression; promoter; targeted biomarker

 DESCRIPTION (provided by applicant): T cell histone GlcNAcylation participates in the epigenetics of lupus ABSTRACT Systemic Lupus Erythematosus (SLE) is a chronic autoimmune disease that affects women ten times more often than men. Altered T cell signaling links genetic and environmental factors and contributes to disease etiopathogenesis. DNA methylation, histone modification, and miRNA regulate gene expression and chromatin structure by modifying the epigenome. DNA methylation suppresses gene transcription and in SLE, the female inactive X-chromosome is hypomethylated, which causes overexpression of genes that predispose females to lupus. SLE is also characterized by global T cell DNA hypomethylation that causes overexpression of immune- related genes and subsequent autoimmunity. We recently found that OGT (O-linked N-acetylglucosamine transferase), an X-linked gene, is overexpressed in female lupus T cells. OGT reversibly adds ß-N-acetyl-glucosamine (O-GlcNAc) to serine and threonine residues of proteins competing with phosphorylation. This makes OGT a regulator of cell signaling and transcription. Interestingly, GlcNAcylated protein levels are increased in female, but not male, T cell lupus patients, which correlate with OGT overexpression. Furthermore, O-GlcNAc is considered part of the histone code, and OGT regulates O-GlcNAcylation of histones. Histone 2B (H2B) is GlcNAc at Ser 112, a modification that facilitates H2BK120 ubiquitination required for transcriptional activation. Additionally, Ten Eleven Translocation enzymes TET2 and TET3 interact directly with OGT and co-localize on chromatin at active promoters. The effects of OGT in signaling pathways and on chromatin structure of T cells are unknown but may play an important role in T cell dysfunction in lupus as well as autoimmunity in general. We hypothesize that OGT overexpression in female lupus T cells modifies signaling pathways and DNA- histone binding profiles by O-GlcNAc of protein targets and chromatin remodelers. Hence, OGT may ultimately be an epigenetic modulator in lupus. To test this hypothesis, we propose to use proteomic and genetic approaches to: 1) Identify molecular targets of OGT, which are key proteins in T cell signaling that may contribute to the pathogenesis of lupus; 2) Determine whether overexpression of OGT in CD4 T cells results in altered glycosylation of histone proteins; and 3) Examine the effects of H2B modifications on gene regulation in cells that overexpress OGT This study will uncover abnormalities in T cell pathways and changes in gene regulation in SLE caused by OGT, a gene aberrantly expressed in female lupus T cells that may predispose females to the disease. By identifying new biomarkers and targets this project will serve as the foundation for future studies aimed at improving therapies for patients suffering from SLE and potentially other autoimmune diseases.