Identification of a common lupus disease-associated microRNA expression pattern in three different murine models of lupus.

Identification of a common lupus disease-associated microRNA expression pattern in three different murine models of lupus.

Recent reports have shown that microRNAs (miRNAs) regulate vital immunological processes and have emerged as key regulators of immune system development and function. Therefore, it is important to determine miRNA dysregulation and its pathogenic contribution in autoimmune diseases, an aspect not ade...

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Main Authors: Rujuan Dai, Yan Zhang, Deena Khan, Bettina Heid, David Caudell, Oswald Crasta, S Ansar Ahmed
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2010-12-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3000827?pdf=render
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spelling doaj-acb7c9a30655470eb4b273064e73c8c62020-11-25T01:45:10ZengPublic Library of Science (PLoS)PLoS ONE1932-62032010-12-01512e1430210.1371/journal.pone.0014302Identification of a common lupus disease-associated microRNA expression pattern in three different murine models of lupus.Rujuan DaiYan ZhangDeena KhanBettina HeidDavid CaudellOswald CrastaS Ansar AhmedRecent reports have shown that microRNAs (miRNAs) regulate vital immunological processes and have emerged as key regulators of immune system development and function. Therefore, it is important to determine miRNA dysregulation and its pathogenic contribution in autoimmune diseases, an aspect not adequately addressed thus far.In this study, we profiled miRNA expressions in splenic lymphocytes from three murine lupus models (MRL-lpr, B6-lpr and NZB/W(F₁)) with different genetic background by miRNA microarray assays and Real-time RT-PCR. Despite the genetic differences among these three lupus stains, a common set of dysregulated miRNAs (miR-182-96-183 cluster, miR-31, and miR-155) was identified in splenocytes when compared with age-matched control mice. The association of these miRNAs with the disease was highlighted by our observation that this miRNA expression pattern was evident in NZB/W mice only at an age when lupus disease is manifested. Further, we have shown that the miRNA dysregulation in MRL-lpr mice was not simply due to the activation of splenocytes. By Real-time RT-PCR, we confirmed that these miRNAs were upregulated in both purified splenic B and T cells from MRL-lpr mice. miR-127 and miR-379, which were greatly upregulated in splenocytes from lpr mice, were moderately increased in diseased NZB/W mice. In addition, Real-time RT-PCR revealed that miR-146a, miR-101a, and miR-17-92 were also markedly upregulated in splenic T, but not B cells from MRL-lpr mice.The identification of common lupus disease-associated miRNAs now forms the basis for the further investigation of the pathogenic contribution of these miRNAs in autoimmune lupus, which will advance our knowledge of the role of miRNAs in autoimmunity. Given that miRNAs are conserved, with regard to both evolution and function, our observation of a common lupus disease-associated miRNA expression pattern in murine lupus models is likely to have significant pathogenic, diagnostic, and/or therapeutic implications in human lupus.http://europepmc.org/articles/PMC3000827?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Rujuan Dai
Yan Zhang
Deena Khan
Bettina Heid
David Caudell
Oswald Crasta
S Ansar Ahmed
spellingShingle Rujuan Dai
Yan Zhang
Deena Khan
Bettina Heid
David Caudell
Oswald Crasta
S Ansar Ahmed
Identification of a common lupus disease-associated microRNA expression pattern in three different murine models of lupus.
PLoS ONE
author_facet Rujuan Dai
Yan Zhang
Deena Khan
Bettina Heid
David Caudell
Oswald Crasta
S Ansar Ahmed
author_sort Rujuan Dai
title Identification of a common lupus disease-associated microRNA expression pattern in three different murine models of lupus.
title_short Identification of a common lupus disease-associated microRNA expression pattern in three different murine models of lupus.
title_full Identification of a common lupus disease-associated microRNA expression pattern in three different murine models of lupus.
title_fullStr Identification of a common lupus disease-associated microRNA expression pattern in three different murine models of lupus.
title_full_unstemmed Identification of a common lupus disease-associated microRNA expression pattern in three different murine models of lupus.
title_sort identification of a common lupus disease-associated microrna expression pattern in three different murine models of lupus.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2010-12-01
description Recent reports have shown that microRNAs (miRNAs) regulate vital immunological processes and have emerged as key regulators of immune system development and function. Therefore, it is important to determine miRNA dysregulation and its pathogenic contribution in autoimmune diseases, an aspect not adequately addressed thus far.In this study, we profiled miRNA expressions in splenic lymphocytes from three murine lupus models (MRL-lpr, B6-lpr and NZB/W(F₁)) with different genetic background by miRNA microarray assays and Real-time RT-PCR. Despite the genetic differences among these three lupus stains, a common set of dysregulated miRNAs (miR-182-96-183 cluster, miR-31, and miR-155) was identified in splenocytes when compared with age-matched control mice. The association of these miRNAs with the disease was highlighted by our observation that this miRNA expression pattern was evident in NZB/W mice only at an age when lupus disease is manifested. Further, we have shown that the miRNA dysregulation in MRL-lpr mice was not simply due to the activation of splenocytes. By Real-time RT-PCR, we confirmed that these miRNAs were upregulated in both purified splenic B and T cells from MRL-lpr mice. miR-127 and miR-379, which were greatly upregulated in splenocytes from lpr mice, were moderately increased in diseased NZB/W mice. In addition, Real-time RT-PCR revealed that miR-146a, miR-101a, and miR-17-92 were also markedly upregulated in splenic T, but not B cells from MRL-lpr mice.The identification of common lupus disease-associated miRNAs now forms the basis for the further investigation of the pathogenic contribution of these miRNAs in autoimmune lupus, which will advance our knowledge of the role of miRNAs in autoimmunity. Given that miRNAs are conserved, with regard to both evolution and function, our observation of a common lupus disease-associated miRNA expression pattern in murine lupus models is likely to have significant pathogenic, diagnostic, and/or therapeutic implications in human lupus.
url http://europepmc.org/articles/PMC3000827?pdf=render
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