miR‐124, ‐128, and ‐137 Orchestrate Neural Differentiation by Acting on Overlapping Gene Sets Containing a Highly Connected Transcription Factor Network
The ventricular‐subventricular zone harbors neural stem cells (NSCs) that can differentiate into neurons, astrocytes, and oligodendrocytes. This process requires loss of stem cell properties and gain of characteristics associated with differentiated cells. miRNAs function as important drivers of thi...
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Published in | Stem cells (Dayton, Ohio) Vol. 34; no. 1; pp. 220 - 232 |
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Main Authors | , , , , , , , , |
Format | Journal Article |
Language | English |
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United States
Oxford University Press
01.01.2016
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Abstract | The ventricular‐subventricular zone harbors neural stem cells (NSCs) that can differentiate into neurons, astrocytes, and oligodendrocytes. This process requires loss of stem cell properties and gain of characteristics associated with differentiated cells. miRNAs function as important drivers of this transition; miR‐124, ‐128, and ‐137 are among the most relevant ones and have been shown to share commonalities and act as proneurogenic regulators. We conducted biological and genomic analyses to dissect their target repertoire during neurogenesis and tested the hypothesis that they act cooperatively to promote differentiation. To map their target genes, we transfected NSCs with antagomiRs and analyzed differences in their mRNA profile throughout differentiation with respect to controls. This strategy led to the identification of 910 targets for miR‐124, 216 for miR‐128, and 652 for miR‐137. The target sets show extensive overlap. Inspection by gene ontology and network analysis indicated that transcription factors are a major component of these miRNAs target sets. Moreover, several of these transcription factors form a highly interconnected network. Sp1 was determined to be the main node of this network and was further investigated. Our data suggest that miR‐124, ‐128, and ‐137 act synergistically to regulate Sp1 expression. Sp1 levels are dramatically reduced as cells differentiate and silencing of its expression reduced neuronal production and affected NSC viability and proliferation. In summary, our results show that miRNAs can act cooperatively and synergistically to regulate complex biological processes like neurogenesis and that transcription factors are heavily targeted to branch out their regulatory effect. Stem Cells 2016;34:220–232 |
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AbstractList | The ventricular-subventricular zone harbors neural stem cells (NSCs) that can differentiate into neurons, astrocytes, and oligodendrocytes. This process requires loss of stem cell properties and gain of characteristics associated with differentiated cells. miRNAs function as important drivers of this transition; miR-124, -128, and -137 are among the most relevant ones and have been shown to share commonalities and act as proneurogenic regulators. We conducted biological and genomic analyses to dissect their target repertoire during neurogenesis and tested the hypothesis that they act cooperatively to promote differentiation. To map their target genes, we transfected NSCs with antagomiRs and analyzed differences in their mRNA profile throughout differentiation with respect to controls. This strategy led to the identification of 910 targets for miR-124, 216 for miR-128, and 652 for miR-137. The target sets show extensive overlap. Inspection by gene ontology and network analysis indicated that transcription factors are a major component of these miRNAs target sets. Moreover, several of these transcription factors form a highly interconnected network. Sp1 was determined to be the main node of this network and was further investigated. Our data suggest that miR-124, -128, and -137 act synergistically to regulate Sp1 expression. Sp1 levels are dramatically reduced as cells differentiate and silencing of its expression reduced neuronal production and affected NSC viability and proliferation. In summary, our results show that miRNAs can act cooperatively and synergistically to regulate complex biological processes like neurogenesis and that transcription factors are heavily targeted to branch out their regulatory effect. The ventricular‐subventricular zone harbors neural stem cells (NSCs) that can differentiate into neurons, astrocytes, and oligodendrocytes. This process requires loss of stem cell properties and gain of characteristics associated with differentiated cells. miRNAs function as important drivers of this transition; miR‐124, ‐128, and ‐137 are among the most relevant ones and have been shown to share commonalities and act as proneurogenic regulators. We conducted biological and genomic analyses to dissect their target repertoire during neurogenesis and tested the hypothesis that they act cooperatively to promote differentiation. To map their target genes, we transfected NSCs with antagomiRs and analyzed differences in their mRNA profile throughout differentiation with respect to controls. This strategy led to the identification of 910 targets for miR‐124, 216 for miR‐128, and 652 for miR‐137. The target sets show extensive overlap. Inspection by gene ontology and network analysis indicated that transcription factors are a major component of these miRNAs target sets. Moreover, several of these transcription factors form a highly interconnected network. Sp1 was determined to be the main node of this network and was further investigated. Our data suggest that miR‐124, ‐128, and ‐137 act synergistically to regulate Sp1 expression. Sp1 levels are dramatically reduced as cells differentiate and silencing of its expression reduced neuronal production and affected NSC viability and proliferation. In summary, our results show that miRNAs can act cooperatively and synergistically to regulate complex biological processes like neurogenesis and that transcription factors are heavily targeted to branch out their regulatory effect. Stem Cells 2016;34:220–232 Abstract The ventricular-subventricular zone harbors neural stem cells (NSCs) that can differentiate into neurons, astrocytes, and oligodendrocytes. This process requires loss of stem cell properties and gain of characteristics associated with differentiated cells. miRNAs function as important drivers of this transition; miR-124, -128, and -137 are among the most relevant ones and have been shown to share commonalities and act as proneurogenic regulators. We conducted biological and genomic analyses to dissect their target repertoire during neurogenesis and tested the hypothesis that they act cooperatively to promote differentiation. To map their target genes, we transfected NSCs with antagomiRs and analyzed differences in their mRNA profile throughout differentiation with respect to controls. This strategy led to the identification of 910 targets for miR-124, 216 for miR-128, and 652 for miR-137. The target sets show extensive overlap. Inspection by gene ontology and network analysis indicated that transcription factors are a major component of these miRNAs target sets. Moreover, several of these transcription factors form a highly interconnected network. Sp1 was determined to be the main node of this network and was further investigated. Our data suggest that miR-124, -128, and -137 act synergistically to regulate Sp1 expression. Sp1 levels are dramatically reduced as cells differentiate and silencing of its expression reduced neuronal production and affected NSC viability and proliferation. In summary, our results show that miRNAs can act cooperatively and synergistically to regulate complex biological processes like neurogenesis and that transcription factors are heavily targeted to branch out their regulatory effect. |
Author | Qiao, Mei Ferreira, Marco A. R. Kokovay, Erzsebet Tegge, Allison N. Penalva, Luiz O. F. Santos, Márcia C. T. Kohnke, Luana Q. Correa, Bruna R. Mahesula, Swetha |
Author_xml | – sequence: 1 givenname: Márcia C. T. surname: Santos fullname: Santos, Márcia C. T. organization: University of Texas Health Science Center at San Antonio – sequence: 2 givenname: Allison N. surname: Tegge fullname: Tegge, Allison N. organization: Virginia Tech – sequence: 3 givenname: Bruna R. surname: Correa fullname: Correa, Bruna R. organization: Centro de Oncologia Molecular, Hospital Sírio‐Libanês – sequence: 4 givenname: Swetha surname: Mahesula fullname: Mahesula, Swetha organization: University of Texas Health Science Center at San Antonio – sequence: 5 givenname: Luana Q. surname: Kohnke fullname: Kohnke, Luana Q. organization: University of Texas Health Science Center at San Antonio – sequence: 6 givenname: Mei surname: Qiao fullname: Qiao, Mei organization: University of Texas Health Science Center at San Antonio – sequence: 7 givenname: Marco A. R. surname: Ferreira fullname: Ferreira, Marco A. R. organization: Virginia Tech – sequence: 8 givenname: Erzsebet surname: Kokovay fullname: Kokovay, Erzsebet organization: University of Texas Health Science Center at San Antonio – sequence: 9 givenname: Luiz O. F. surname: Penalva fullname: Penalva, Luiz O. F. organization: University of Texas Health Science Center at San Antonio |
BackLink | https://www.ncbi.nlm.nih.gov/pubmed/26369286$$D View this record in MEDLINE/PubMed |
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Keywords | Transcription factors miR-137 mir-124 Sp1 Neural stem cell miRNA Differentiation miR-128 Neurogenesis |
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Snippet | The ventricular‐subventricular zone harbors neural stem cells (NSCs) that can differentiate into neurons, astrocytes, and oligodendrocytes. This process... The ventricular-subventricular zone harbors neural stem cells (NSCs) that can differentiate into neurons, astrocytes, and oligodendrocytes. This process... Abstract The ventricular-subventricular zone harbors neural stem cells (NSCs) that can differentiate into neurons, astrocytes, and oligodendrocytes. This... |
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SubjectTerms | Animals Cell Differentiation - genetics Cell Proliferation Cell Self Renewal Differentiation Gene Expression Regulation Gene Regulatory Networks Genes Genome Humans Mice MicroRNAs - genetics MicroRNAs - metabolism miRNA mir‐124 miR‐128 miR‐137 Neural stem cell Neural Stem Cells - cytology Neurogenesis Neurons - cytology Neurons - metabolism Oligonucleotides, Antisense - metabolism Sequence Analysis, RNA Sp1 Sp1 Transcription Factor - metabolism Stem cells Transcription factors Transfection |
Title | miR‐124, ‐128, and ‐137 Orchestrate Neural Differentiation by Acting on Overlapping Gene Sets Containing a Highly Connected Transcription Factor Network |
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