Next-Generation Sequencing Identifies MicroRNAs that Associate with Pathogenic Autoimmune Neuroinflammation in Rats

Bergman, Petra; James, Tojo; Kular, Lara; Ruhrmann, Sabrina; Kramarova, Tatiana V.; Kvist, Anders; Šupić, Gordana; Gillett, Alan; Pivarcsi, Andor; Jagodic, Maja

doi:10.4049/jimmunol.1200728

Cited by 44 publications

(66 citation statements)

References 75 publications

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“…However, the identification of changes in miR‐21 expression in EVs after TBI agrees with increases in whole brain tissue observed by others . Other than TBI, increased expression of miR‐21 has also been observed in many models of neuroinflammation and neuronal injury .…”

Section: Discussionsupporting

confidence: 88%

Traumatic brain injury increases levels of miR‐21 in extracellular vesicles: implications for neuroinflammation

et al. 2016

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Traumatic brain injury (TBI) is an important health concern and effective treatment strategies remain elusive. Understanding the complex multicellular response to TBI may provide new avenues for intervention. In the context of TBI, cell–cell communication is critical. One relatively unexplored form of cell–cell communication in TBI is extracellular vesicles (EVs). These membrane‐bound vesicles can carry many different types of cargo between cells. Recently, miRNA in EVs have been shown to mediate neuroinflammation and neuronal injury. To explore the role of EV‐associated miRNA in TBI, we isolated EVs from the brain of injured mice and controls, purified RNA from brain EVs, and performed miRNA sequencing. We found that the expression of miR‐212 decreased, while miR‐21, miR‐146, miR‐7a, and miR‐7b were significantly increased with injury, with miR‐21 showing the largest change between conditions. The expression of miR‐21 in the brain was primarily localized to neurons near the lesion site. Interestingly, adjacent to these miR‐21‐expressing neurons were activated microglia. The concurrent increase in miR‐21 in EVs with the elevation of miR‐21 in neurons, suggests that miR‐21 is secreted from neurons as potential EV cargo. Thus, this study reveals a new potential mechanism of cell–cell communication not previously described in TBI.

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Section: Discussionsupporting

confidence: 88%

Traumatic brain injury increases levels of miR‐21 in extracellular vesicles: implications for neuroinflammation

et al. 2016

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“…Such reduced threshold of activation of T H 17 cells compared with other T-cell subsets may lead to increased responses to a specific antigen. Of note, miR-181a was recently associated with the susceptibility to develop EAE in rats, showing higher expression in a strain susceptible to EAE compared with an EAE-resistant one 42 , pointing towards a potential role for miR-181a in regulating specific T H 17-cell responses in autoimmunity.…”

Section: Articlementioning

confidence: 99%

ERK phosphorylation and miR-181a expression modulate activation of human memory TH17 cells

et al. 2015

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T helper (T H ) cell polarization during priming is modulated by a number of signals, but whether polarization to a given phenotype also influences recall responses of memory T H cells is relatively unknown. Here we show that miR-181a is selectively induced in both human and mouse naive T cells differentiating into the T H 17, but not T H 1 or T H 2 subset. In human memory T H 17 cells, miR-181a regulates responses to cognate antigens through modulation of ERK phosphorylation. By enhancing the signalling cascade from the T-cell receptor, such molecular network reduces the threshold of T H 17 cell activation. Moreover, at a late time point, the same network induces a self-regulatory mechanism dependent on ID3, a negative regulator of transcription factors that control RORC expression, thus modulating T H 17 activity. Our results demonstrate that the phenotype acquired by T H cells during priming contributes to their threshold of activation to secondary antigenic stimulations, thus influencing memory responses.

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“…Bergman et al have demonstrated that the PRKCD gene is a direct target of miR-181a in a rat model of multiple sclerosis. 47 Ke et al and Chen et al found that miR-181a could inhibit the irradiation-and cisplatininduced apoptosis of human squamous cervical carcinoma cells via downregulating the expression levels of PRKCD. 48,49 PBX3 PBX3, a HOXA cofactor gene, can encode pre-B-cell leukemia transcription factor 3, which is capable of regulating the transcription of downstream targets by forming stable heterocomplexes with HOX and MEIS proteins.…”

Section: Protein Kinase C Delta Typementioning

confidence: 99%

Role of miR-181a in the process of apoptosis of multiple malignant tumors: A literature review

Feng¹,

Zhang²,

Yang³

et al. 2018

Adv Clin Exp Med

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It has been recognized that miR-181a expression is dysregulated and intimately associated with clinical prognosis in a variety of human cancers. However, the direct role of miR-181a in tumor progression has been elusive. Moreover, mounting evidence has demonstrated that cellular apoptosis, a physiological process of programmed cell death, is disrupted in various categories of human malignancies. Multiple apoptosisrelated genes have been proven to act as the target genes of miR-181a. In this study, we hypothesize that miR-181a probably plays a potential role in modulating the procession and apoptosis of cancer cells. We performed a literature review and elucidated how miR-181a modulated cellular apoptosis, especially the malignant neoplasm cells. We also unraveled the potential role of miR-181a in the diagnosis, treatment and clinical prognosis of multiple human malignancies - miR-181a plays a pivotal role in the development, treatment and prognosis of patients suffering from malignant tumors. It also participates in the development of cancer partially by modulating cellular apoptosis.

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Next-Generation Sequencing Identifies MicroRNAs that Associate with Pathogenic Autoimmune Neuroinflammation in Rats

Cited by 44 publications

References 75 publications

Traumatic brain injury increases levels of miR‐21 in extracellular vesicles: implications for neuroinflammation

Traumatic brain injury increases levels of miR‐21 in extracellular vesicles: implications for neuroinflammation

ERK phosphorylation and miR-181a expression modulate activation of human memory TH17 cells

Role of miR-181a in the process of apoptosis of multiple malignant tumors: A literature review

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