Nucleic Acid-Sensing and Interferon-Inducible Pathways Show Differential Methylation in MZ Twins Discordant for Lupus and Overexpression in Independent Lupus Samples: Implications for Pathogenic Mechanism and Drug Targeting

Systemic lupus erythematosus (SLE) is a chronic, multisystem, autoimmune inflammatory disease with genomic and non-genomic contributions to risk. We hypothesize that epigenetic factors are a significant contributor to SLE risk and may be informative for identifying pathogenic mechanisms and therapeu...

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Autores principales: Marion, Miranda C., Ramos, Paula S., Bachali, Prathyusha, Labonte, Adam C., Zimmerman, Kip D., Ainsworth, Hannah C., Heuer, Sarah E., Robl, Robert D., Catalina, Michelle D., Kelly, Jennifer A., Howard, Timothy D., Lipsky, Peter E., Grammer, Amrie C., Langefeld, Carl D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8701117/
https://www.ncbi.nlm.nih.gov/pubmed/34946847
http://dx.doi.org/10.3390/genes12121898
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author Marion, Miranda C.
Ramos, Paula S.
Bachali, Prathyusha
Labonte, Adam C.
Zimmerman, Kip D.
Ainsworth, Hannah C.
Heuer, Sarah E.
Robl, Robert D.
Catalina, Michelle D.
Kelly, Jennifer A.
Howard, Timothy D.
Lipsky, Peter E.
Grammer, Amrie C.
Langefeld, Carl D.
author_facet Marion, Miranda C.
Ramos, Paula S.
Bachali, Prathyusha
Labonte, Adam C.
Zimmerman, Kip D.
Ainsworth, Hannah C.
Heuer, Sarah E.
Robl, Robert D.
Catalina, Michelle D.
Kelly, Jennifer A.
Howard, Timothy D.
Lipsky, Peter E.
Grammer, Amrie C.
Langefeld, Carl D.
author_sort Marion, Miranda C.
collection PubMed
description Systemic lupus erythematosus (SLE) is a chronic, multisystem, autoimmune inflammatory disease with genomic and non-genomic contributions to risk. We hypothesize that epigenetic factors are a significant contributor to SLE risk and may be informative for identifying pathogenic mechanisms and therapeutic targets. To test this hypothesis while controlling for genetic background, we performed an epigenome-wide analysis of DNA methylation in genomic DNA from whole blood in three pairs of female monozygotic (MZ) twins of European ancestry, discordant for SLE. Results were replicated on the same array in four cell types from a set of four Danish female MZ twin pairs discordant for SLE. Genes implicated by the epigenetic analyses were then evaluated in 10 independent SLE gene expression datasets from the Gene Expression Omnibus (GEO). There were 59 differentially methylated loci between unaffected and affected MZ twins in whole blood, including 11 novel loci. All but two of these loci were hypomethylated in the SLE twins relative to the unaffected twins. The genes harboring these hypomethylated loci exhibited increased expression in multiple independent datasets of SLE patients. This pattern was largely consistent regardless of disease activity, cell type, or renal tissue type. The genes proximal to CpGs exhibiting differential methylation (DM) in the SLE-discordant MZ twins and exhibiting differential expression (DE) in independent SLE GEO cohorts (DM-DE genes) clustered into two pathways: the nucleic acid-sensing pathway and the type I interferon pathway. The DM-DE genes were also informatically queried for potential gene–drug interactions, yielding a list of 41 drugs including a known SLE therapy. The DM-DE genes delineate two important biologic pathways that are not only reflective of the heterogeneity of SLE but may also correlate with distinct IFN responses that depend on the source, type, and location of nucleic acid molecules and the activated receptors in individual patients. Cell- and tissue-specific analyses will be critical to the understanding of genetic factors dysregulating the nucleic acid-sensing and IFN pathways and whether these factors could be appropriate targets for therapeutic intervention.
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spelling pubmed-87011172021-12-24 Nucleic Acid-Sensing and Interferon-Inducible Pathways Show Differential Methylation in MZ Twins Discordant for Lupus and Overexpression in Independent Lupus Samples: Implications for Pathogenic Mechanism and Drug Targeting Marion, Miranda C. Ramos, Paula S. Bachali, Prathyusha Labonte, Adam C. Zimmerman, Kip D. Ainsworth, Hannah C. Heuer, Sarah E. Robl, Robert D. Catalina, Michelle D. Kelly, Jennifer A. Howard, Timothy D. Lipsky, Peter E. Grammer, Amrie C. Langefeld, Carl D. Genes (Basel) Article Systemic lupus erythematosus (SLE) is a chronic, multisystem, autoimmune inflammatory disease with genomic and non-genomic contributions to risk. We hypothesize that epigenetic factors are a significant contributor to SLE risk and may be informative for identifying pathogenic mechanisms and therapeutic targets. To test this hypothesis while controlling for genetic background, we performed an epigenome-wide analysis of DNA methylation in genomic DNA from whole blood in three pairs of female monozygotic (MZ) twins of European ancestry, discordant for SLE. Results were replicated on the same array in four cell types from a set of four Danish female MZ twin pairs discordant for SLE. Genes implicated by the epigenetic analyses were then evaluated in 10 independent SLE gene expression datasets from the Gene Expression Omnibus (GEO). There were 59 differentially methylated loci between unaffected and affected MZ twins in whole blood, including 11 novel loci. All but two of these loci were hypomethylated in the SLE twins relative to the unaffected twins. The genes harboring these hypomethylated loci exhibited increased expression in multiple independent datasets of SLE patients. This pattern was largely consistent regardless of disease activity, cell type, or renal tissue type. The genes proximal to CpGs exhibiting differential methylation (DM) in the SLE-discordant MZ twins and exhibiting differential expression (DE) in independent SLE GEO cohorts (DM-DE genes) clustered into two pathways: the nucleic acid-sensing pathway and the type I interferon pathway. The DM-DE genes were also informatically queried for potential gene–drug interactions, yielding a list of 41 drugs including a known SLE therapy. The DM-DE genes delineate two important biologic pathways that are not only reflective of the heterogeneity of SLE but may also correlate with distinct IFN responses that depend on the source, type, and location of nucleic acid molecules and the activated receptors in individual patients. Cell- and tissue-specific analyses will be critical to the understanding of genetic factors dysregulating the nucleic acid-sensing and IFN pathways and whether these factors could be appropriate targets for therapeutic intervention. MDPI 2021-11-26 /pmc/articles/PMC8701117/ /pubmed/34946847 http://dx.doi.org/10.3390/genes12121898 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Marion, Miranda C.
Ramos, Paula S.
Bachali, Prathyusha
Labonte, Adam C.
Zimmerman, Kip D.
Ainsworth, Hannah C.
Heuer, Sarah E.
Robl, Robert D.
Catalina, Michelle D.
Kelly, Jennifer A.
Howard, Timothy D.
Lipsky, Peter E.
Grammer, Amrie C.
Langefeld, Carl D.
Nucleic Acid-Sensing and Interferon-Inducible Pathways Show Differential Methylation in MZ Twins Discordant for Lupus and Overexpression in Independent Lupus Samples: Implications for Pathogenic Mechanism and Drug Targeting
title Nucleic Acid-Sensing and Interferon-Inducible Pathways Show Differential Methylation in MZ Twins Discordant for Lupus and Overexpression in Independent Lupus Samples: Implications for Pathogenic Mechanism and Drug Targeting
title_full Nucleic Acid-Sensing and Interferon-Inducible Pathways Show Differential Methylation in MZ Twins Discordant for Lupus and Overexpression in Independent Lupus Samples: Implications for Pathogenic Mechanism and Drug Targeting
title_fullStr Nucleic Acid-Sensing and Interferon-Inducible Pathways Show Differential Methylation in MZ Twins Discordant for Lupus and Overexpression in Independent Lupus Samples: Implications for Pathogenic Mechanism and Drug Targeting
title_full_unstemmed Nucleic Acid-Sensing and Interferon-Inducible Pathways Show Differential Methylation in MZ Twins Discordant for Lupus and Overexpression in Independent Lupus Samples: Implications for Pathogenic Mechanism and Drug Targeting
title_short Nucleic Acid-Sensing and Interferon-Inducible Pathways Show Differential Methylation in MZ Twins Discordant for Lupus and Overexpression in Independent Lupus Samples: Implications for Pathogenic Mechanism and Drug Targeting
title_sort nucleic acid-sensing and interferon-inducible pathways show differential methylation in mz twins discordant for lupus and overexpression in independent lupus samples: implications for pathogenic mechanism and drug targeting
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8701117/
https://www.ncbi.nlm.nih.gov/pubmed/34946847
http://dx.doi.org/10.3390/genes12121898
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