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Transcriptional Signatures as a Disease-Specific and Predictive Inflammatory Biomarker for Type 1 Diabetes

The complex milieu of inflammatory mediators associated with many diseases is often too dilute to directly measure in the periphery, necessitating development of more sensitive measurements suitable for mechanistic studies, earlier diagnosis, guiding therapeutic decisions, and monitoring interventio...

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Autores principales: Levy, Hara, Wang, Xujing, Kaldunski, Mary, Jia, Shuang, Kramer, Joanna, Pavletich, Scott J., Reske, Melissa, Gessel, Trevor, Yassai, Maryam, Quasney, Michael W., Dahmer, Mary K., Gorski, Jack, Hessner, Martin J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4265236/
https://www.ncbi.nlm.nih.gov/pubmed/22972474
http://dx.doi.org/10.1038/gene.2012.41
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author Levy, Hara
Wang, Xujing
Kaldunski, Mary
Jia, Shuang
Kramer, Joanna
Pavletich, Scott J.
Reske, Melissa
Gessel, Trevor
Yassai, Maryam
Quasney, Michael W.
Dahmer, Mary K.
Gorski, Jack
Hessner, Martin J.
author_facet Levy, Hara
Wang, Xujing
Kaldunski, Mary
Jia, Shuang
Kramer, Joanna
Pavletich, Scott J.
Reske, Melissa
Gessel, Trevor
Yassai, Maryam
Quasney, Michael W.
Dahmer, Mary K.
Gorski, Jack
Hessner, Martin J.
author_sort Levy, Hara
collection PubMed
description The complex milieu of inflammatory mediators associated with many diseases is often too dilute to directly measure in the periphery, necessitating development of more sensitive measurements suitable for mechanistic studies, earlier diagnosis, guiding therapeutic decisions, and monitoring interventions. We previously demonstrated that plasma samples from recent-onset Type 1 diabetes (RO T1D) patients induce a proinflammatory transcriptional signature in freshly drawn peripheral blood mononuclear cells (PBMCs) relative to that of unrelated healthy controls (HC). Here, using cryopreserved PBMC, we analyzed larger RO T1D and HC cohorts, examined T1D progression in pre-onset samples, and compared the RO T1D signature to those associated with three disorders characterized by airway infection and inflammation. The RO T1D signature, consisting of interleukin-1 cytokine family members, chemokines involved in immunocyte chemotaxis, immune receptors, and signaling molecules, was detected during early pre-diabetes and found to resolve post-onset. The signatures associated with cystic fibrosis patients chronically infected with Pseudomonas aeruginosa, patients with confirmed bacterial pneumonia, and subjects with H1N1 influenza all reflected immunological activation, yet each were distinct from one another and negatively correlated with that of T1D. This study highlights the remarkable capacity of cells to serve as biosensors capable of sensitively and comprehensively differentiating immunological states.
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spelling pubmed-42652362014-12-13 Transcriptional Signatures as a Disease-Specific and Predictive Inflammatory Biomarker for Type 1 Diabetes Levy, Hara Wang, Xujing Kaldunski, Mary Jia, Shuang Kramer, Joanna Pavletich, Scott J. Reske, Melissa Gessel, Trevor Yassai, Maryam Quasney, Michael W. Dahmer, Mary K. Gorski, Jack Hessner, Martin J. Genes Immun Article The complex milieu of inflammatory mediators associated with many diseases is often too dilute to directly measure in the periphery, necessitating development of more sensitive measurements suitable for mechanistic studies, earlier diagnosis, guiding therapeutic decisions, and monitoring interventions. We previously demonstrated that plasma samples from recent-onset Type 1 diabetes (RO T1D) patients induce a proinflammatory transcriptional signature in freshly drawn peripheral blood mononuclear cells (PBMCs) relative to that of unrelated healthy controls (HC). Here, using cryopreserved PBMC, we analyzed larger RO T1D and HC cohorts, examined T1D progression in pre-onset samples, and compared the RO T1D signature to those associated with three disorders characterized by airway infection and inflammation. The RO T1D signature, consisting of interleukin-1 cytokine family members, chemokines involved in immunocyte chemotaxis, immune receptors, and signaling molecules, was detected during early pre-diabetes and found to resolve post-onset. The signatures associated with cystic fibrosis patients chronically infected with Pseudomonas aeruginosa, patients with confirmed bacterial pneumonia, and subjects with H1N1 influenza all reflected immunological activation, yet each were distinct from one another and negatively correlated with that of T1D. This study highlights the remarkable capacity of cells to serve as biosensors capable of sensitively and comprehensively differentiating immunological states. 2012-09-13 2012-12 /pmc/articles/PMC4265236/ /pubmed/22972474 http://dx.doi.org/10.1038/gene.2012.41 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Levy, Hara
Wang, Xujing
Kaldunski, Mary
Jia, Shuang
Kramer, Joanna
Pavletich, Scott J.
Reske, Melissa
Gessel, Trevor
Yassai, Maryam
Quasney, Michael W.
Dahmer, Mary K.
Gorski, Jack
Hessner, Martin J.
Transcriptional Signatures as a Disease-Specific and Predictive Inflammatory Biomarker for Type 1 Diabetes
title Transcriptional Signatures as a Disease-Specific and Predictive Inflammatory Biomarker for Type 1 Diabetes
title_full Transcriptional Signatures as a Disease-Specific and Predictive Inflammatory Biomarker for Type 1 Diabetes
title_fullStr Transcriptional Signatures as a Disease-Specific and Predictive Inflammatory Biomarker for Type 1 Diabetes
title_full_unstemmed Transcriptional Signatures as a Disease-Specific and Predictive Inflammatory Biomarker for Type 1 Diabetes
title_short Transcriptional Signatures as a Disease-Specific and Predictive Inflammatory Biomarker for Type 1 Diabetes
title_sort transcriptional signatures as a disease-specific and predictive inflammatory biomarker for type 1 diabetes
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4265236/
https://www.ncbi.nlm.nih.gov/pubmed/22972474
http://dx.doi.org/10.1038/gene.2012.41
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