MicroRNA-30a controls the instability of inducible [CD4.sup.+] Tregs through SOCS1
Inducible regulatory T cells (iTregs) are an important subset of Tregs and play a role in the maintenance of peripheral tolerance, and the occurrence of a number of diseases, including tumors and autoimmune diseases. However, the instability of iTregs is a major obstacle for their potential applicat...
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| Veröffentlicht in: | Molecular medicine reports 2019-11, Vol.20 (5), p.4303 |
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| creator | Zhou, Ya Li, Yongju Lu, Jia Hong, Xiaowu Xu, Lin |
| description | Inducible regulatory T cells (iTregs) are an important subset of Tregs and play a role in the maintenance of peripheral tolerance, and the occurrence of a number of diseases, including tumors and autoimmune diseases. However, the instability of iTregs is a major obstacle for their potential application in clinical trials. The underlying mechanism of iTreg instability remains largely unknown. In the present study, the expression level of microRNA (miRNA/miR)-30a in murine iTregs was evaluated using reverse transcription-quantitative PCR. miR-30a mimics and a miR-negative control (NC) were transiently transfected into iTregs using Nucleofector technology. The effects of miR-30a on the suppressive function of murine iTregs in vitro and in vivo were investigated using MTT, adoptive cell transfer (ACT) and flow cytometry assays, as well as a murine model of lung cancer. In the present study, it was identified that the expression level of miR-30a was lower in murine iTregs in vitro compared with natural (n)Tregs. Furthermore, compared with miR-NC, miR-30a mimics impaired the suppressive function of murine iTregs on murine [CD4.sup.+] T cell proliferation in vitro, which was accompanied by the altered expression of cytotoxic T lymphocyte-associated antigen 4 and glucocorticoid induced tumor necrosis factor receptor, as well as transforming growth factor-[beta] and interleukin-10. It was also observed that, compared with miR-NC, miR-30a mimics abrogated the suppressive effects of murine iTregs on murine [CD8.sup.+] T cell function in vivo, producing an effective antitumor effect in mice bearing 3LL lung cancer cells in the ACT assay. From a mechanistic point, the expression level of suppressor of cytokine signaling 1, a putative target of miR-30a, was elevated, altering the activation of the Akt and STAT1 pathway in the miR-30a mimic transfected group compared with the miR-NC group, reducing the suppressive function of murine iTregs. The present study identified a role for miR-30a in the instability of iTregs and provided a novel insight into the development of therapeutic strategies for promoting T-cell immunity via the regulation of iTreg instability by targeting specific miRNAs. Key words: [CD4.sup.+][Foxp3.sup.+] Treg cells, microRNA-30a, lung cancer, SOSC1, TGF-[beta] |
| doi_str_mv | 10.3892/mmr.2019.10666 |
| format | Article |
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However, the instability of iTregs is a major obstacle for their potential application in clinical trials. The underlying mechanism of iTreg instability remains largely unknown. In the present study, the expression level of microRNA (miRNA/miR)-30a in murine iTregs was evaluated using reverse transcription-quantitative PCR. miR-30a mimics and a miR-negative control (NC) were transiently transfected into iTregs using Nucleofector technology. The effects of miR-30a on the suppressive function of murine iTregs in vitro and in vivo were investigated using MTT, adoptive cell transfer (ACT) and flow cytometry assays, as well as a murine model of lung cancer. In the present study, it was identified that the expression level of miR-30a was lower in murine iTregs in vitro compared with natural (n)Tregs. Furthermore, compared with miR-NC, miR-30a mimics impaired the suppressive function of murine iTregs on murine [CD4.sup.+] T cell proliferation in vitro, which was accompanied by the altered expression of cytotoxic T lymphocyte-associated antigen 4 and glucocorticoid induced tumor necrosis factor receptor, as well as transforming growth factor-[beta] and interleukin-10. It was also observed that, compared with miR-NC, miR-30a mimics abrogated the suppressive effects of murine iTregs on murine [CD8.sup.+] T cell function in vivo, producing an effective antitumor effect in mice bearing 3LL lung cancer cells in the ACT assay. From a mechanistic point, the expression level of suppressor of cytokine signaling 1, a putative target of miR-30a, was elevated, altering the activation of the Akt and STAT1 pathway in the miR-30a mimic transfected group compared with the miR-NC group, reducing the suppressive function of murine iTregs. The present study identified a role for miR-30a in the instability of iTregs and provided a novel insight into the development of therapeutic strategies for promoting T-cell immunity via the regulation of iTreg instability by targeting specific miRNAs. Key words: [CD4.sup.+][Foxp3.sup.+] Treg cells, microRNA-30a, lung cancer, SOSC1, TGF-[beta]</description><identifier>ISSN: 1791-2997</identifier><identifier>DOI: 10.3892/mmr.2019.10666</identifier><language>eng</language><publisher>Spandidos Publications</publisher><subject>Antigens ; Autoimmune diseases ; Biotechnology industries ; Bone morphogenetic proteins ; Cancer ; Cancer cells ; Clinical trials ; Glucocorticoids ; Interleukins ; Lung cancer ; Lymphocytes ; MicroRNA ; Necrosis ; Polymerase chain reaction ; Scientific equipment industry ; T cells ; Technology ; Transcription (Genetics) ; Transforming growth factors ; Tumors</subject><ispartof>Molecular medicine reports, 2019-11, Vol.20 (5), p.4303</ispartof><rights>COPYRIGHT 2019 Spandidos Publications</rights><woscitedreferencessubscribed>false</woscitedreferencessubscribed></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,776,780,27901,27902</link.rule.ids></links><search><creatorcontrib>Zhou, Ya</creatorcontrib><creatorcontrib>Li, Yongju</creatorcontrib><creatorcontrib>Lu, Jia</creatorcontrib><creatorcontrib>Hong, Xiaowu</creatorcontrib><creatorcontrib>Xu, Lin</creatorcontrib><title>MicroRNA-30a controls the instability of inducible [CD4.sup.+] Tregs through SOCS1</title><title>Molecular medicine reports</title><description>Inducible regulatory T cells (iTregs) are an important subset of Tregs and play a role in the maintenance of peripheral tolerance, and the occurrence of a number of diseases, including tumors and autoimmune diseases. However, the instability of iTregs is a major obstacle for their potential application in clinical trials. The underlying mechanism of iTreg instability remains largely unknown. In the present study, the expression level of microRNA (miRNA/miR)-30a in murine iTregs was evaluated using reverse transcription-quantitative PCR. miR-30a mimics and a miR-negative control (NC) were transiently transfected into iTregs using Nucleofector technology. The effects of miR-30a on the suppressive function of murine iTregs in vitro and in vivo were investigated using MTT, adoptive cell transfer (ACT) and flow cytometry assays, as well as a murine model of lung cancer. In the present study, it was identified that the expression level of miR-30a was lower in murine iTregs in vitro compared with natural (n)Tregs. Furthermore, compared with miR-NC, miR-30a mimics impaired the suppressive function of murine iTregs on murine [CD4.sup.+] T cell proliferation in vitro, which was accompanied by the altered expression of cytotoxic T lymphocyte-associated antigen 4 and glucocorticoid induced tumor necrosis factor receptor, as well as transforming growth factor-[beta] and interleukin-10. It was also observed that, compared with miR-NC, miR-30a mimics abrogated the suppressive effects of murine iTregs on murine [CD8.sup.+] T cell function in vivo, producing an effective antitumor effect in mice bearing 3LL lung cancer cells in the ACT assay. From a mechanistic point, the expression level of suppressor of cytokine signaling 1, a putative target of miR-30a, was elevated, altering the activation of the Akt and STAT1 pathway in the miR-30a mimic transfected group compared with the miR-NC group, reducing the suppressive function of murine iTregs. The present study identified a role for miR-30a in the instability of iTregs and provided a novel insight into the development of therapeutic strategies for promoting T-cell immunity via the regulation of iTreg instability by targeting specific miRNAs. Key words: [CD4.sup.+][Foxp3.sup.+] Treg cells, microRNA-30a, lung cancer, SOSC1, TGF-[beta]</description><subject>Antigens</subject><subject>Autoimmune diseases</subject><subject>Biotechnology industries</subject><subject>Bone morphogenetic proteins</subject><subject>Cancer</subject><subject>Cancer cells</subject><subject>Clinical trials</subject><subject>Glucocorticoids</subject><subject>Interleukins</subject><subject>Lung cancer</subject><subject>Lymphocytes</subject><subject>MicroRNA</subject><subject>Necrosis</subject><subject>Polymerase chain reaction</subject><subject>Scientific equipment industry</subject><subject>T cells</subject><subject>Technology</subject><subject>Transcription (Genetics)</subject><subject>Transforming growth factors</subject><subject>Tumors</subject><issn>1791-2997</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2019</creationdate><recordtype>article</recordtype><sourceid/><recordid>eNptj81LxDAUxHNQcF29eg54lMaXNE2TY6m6CqsLu72JLGk-upF-SNM9-N9b0YMHmcPwht88GISuKJBUKnbbdSNhQBWhIIQ4QQuaK5owpfIzdB7jO4DIWKYWaPsczDhsX4okBY3N0E_j0EY8HRwOfZx0HdowfeLBz6c9mlC3Dr-Wd5zE4we5ecPV6JpvfByOzQHvNuWOXqBTr9voLn99iaqH-6p8TNab1VNZrJNG5CLxVPPMGepEbZWWDnTuvKTaGGsM5JJDTT2rrRaSc2VBMZo5KTUA91zbNF2i65-3jW7dPvR-mEZtuhDNvhCQM5lSJmaK_EPNsq4L81znw5z_KXwBmiheGg</recordid><startdate>20191101</startdate><enddate>20191101</enddate><creator>Zhou, Ya</creator><creator>Li, Yongju</creator><creator>Lu, Jia</creator><creator>Hong, Xiaowu</creator><creator>Xu, Lin</creator><general>Spandidos Publications</general><scope/></search><sort><creationdate>20191101</creationdate><title>MicroRNA-30a controls the instability of inducible [CD4.sup.+] Tregs through SOCS1</title><author>Zhou, Ya ; Li, Yongju ; Lu, Jia ; Hong, Xiaowu ; Xu, Lin</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-g676-f1a45ec1e6bd9a8e0a7ef81accdcc07840b1f2bda68449d09215e88a004f4ad33</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2019</creationdate><topic>Antigens</topic><topic>Autoimmune diseases</topic><topic>Biotechnology industries</topic><topic>Bone morphogenetic proteins</topic><topic>Cancer</topic><topic>Cancer cells</topic><topic>Clinical trials</topic><topic>Glucocorticoids</topic><topic>Interleukins</topic><topic>Lung cancer</topic><topic>Lymphocytes</topic><topic>MicroRNA</topic><topic>Necrosis</topic><topic>Polymerase chain reaction</topic><topic>Scientific equipment industry</topic><topic>T cells</topic><topic>Technology</topic><topic>Transcription (Genetics)</topic><topic>Transforming growth factors</topic><topic>Tumors</topic><toplevel>online_resources</toplevel><creatorcontrib>Zhou, Ya</creatorcontrib><creatorcontrib>Li, Yongju</creatorcontrib><creatorcontrib>Lu, Jia</creatorcontrib><creatorcontrib>Hong, Xiaowu</creatorcontrib><creatorcontrib>Xu, Lin</creatorcontrib><jtitle>Molecular medicine reports</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Zhou, Ya</au><au>Li, Yongju</au><au>Lu, Jia</au><au>Hong, Xiaowu</au><au>Xu, Lin</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>MicroRNA-30a controls the instability of inducible [CD4.sup.+] Tregs through SOCS1</atitle><jtitle>Molecular medicine reports</jtitle><date>2019-11-01</date><risdate>2019</risdate><volume>20</volume><issue>5</issue><spage>4303</spage><pages>4303-</pages><issn>1791-2997</issn><abstract>Inducible regulatory T cells (iTregs) are an important subset of Tregs and play a role in the maintenance of peripheral tolerance, and the occurrence of a number of diseases, including tumors and autoimmune diseases. However, the instability of iTregs is a major obstacle for their potential application in clinical trials. The underlying mechanism of iTreg instability remains largely unknown. In the present study, the expression level of microRNA (miRNA/miR)-30a in murine iTregs was evaluated using reverse transcription-quantitative PCR. miR-30a mimics and a miR-negative control (NC) were transiently transfected into iTregs using Nucleofector technology. The effects of miR-30a on the suppressive function of murine iTregs in vitro and in vivo were investigated using MTT, adoptive cell transfer (ACT) and flow cytometry assays, as well as a murine model of lung cancer. In the present study, it was identified that the expression level of miR-30a was lower in murine iTregs in vitro compared with natural (n)Tregs. Furthermore, compared with miR-NC, miR-30a mimics impaired the suppressive function of murine iTregs on murine [CD4.sup.+] T cell proliferation in vitro, which was accompanied by the altered expression of cytotoxic T lymphocyte-associated antigen 4 and glucocorticoid induced tumor necrosis factor receptor, as well as transforming growth factor-[beta] and interleukin-10. It was also observed that, compared with miR-NC, miR-30a mimics abrogated the suppressive effects of murine iTregs on murine [CD8.sup.+] T cell function in vivo, producing an effective antitumor effect in mice bearing 3LL lung cancer cells in the ACT assay. From a mechanistic point, the expression level of suppressor of cytokine signaling 1, a putative target of miR-30a, was elevated, altering the activation of the Akt and STAT1 pathway in the miR-30a mimic transfected group compared with the miR-NC group, reducing the suppressive function of murine iTregs. The present study identified a role for miR-30a in the instability of iTregs and provided a novel insight into the development of therapeutic strategies for promoting T-cell immunity via the regulation of iTreg instability by targeting specific miRNAs. Key words: [CD4.sup.+][Foxp3.sup.+] Treg cells, microRNA-30a, lung cancer, SOSC1, TGF-[beta]</abstract><pub>Spandidos Publications</pub><doi>10.3892/mmr.2019.10666</doi></addata></record> |
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| source | Spandidos Publications Journals; Elektronische Zeitschriftenbibliothek - Frei zugängliche E-Journals; Alma/SFX Local Collection |
| subjects | Antigens Autoimmune diseases Biotechnology industries Bone morphogenetic proteins Cancer Cancer cells Clinical trials Glucocorticoids Interleukins Lung cancer Lymphocytes MicroRNA Necrosis Polymerase chain reaction Scientific equipment industry T cells Technology Transcription (Genetics) Transforming growth factors Tumors |
| title | MicroRNA-30a controls the instability of inducible [CD4.sup.+] Tregs through SOCS1 |
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