TRPA1–FGFR2 binding event is a regulatory oncogenic driver modulated by miRNA-142-3p

Berrout, Jonathan; Kyriakopoulou, Eleni; Moparthi, Lavanya; Hogea, Alexandra S.; Berrout, Liza; Ivan, Cristina; Lorger, Mihaela; Boyle, John; Peers, Chris; Muench, Stephen P.; Elíes, Jacobo; Hu, Xin; Hurst, Carolyn D.; Hall, Thomas; Umamaheswaran, Sujanitha; Wesley, Laura; Gagea, Mihai; Shires, Michael; Manfield, Iain W.; Knowles, Margaret A.; Davies, Simon P.; Suhling, Klaus; Gonzalez, Yurema Teijeiro; Carragher, Neil O.; MacLeod, Kenneth G.; Abbott, N. Joan; Calin, George A.; Gamper, Nikita; Zygmunt, Peter M.; Timsah, Zahra

doi:10.1038/s41467-017-00983-w

Cited by 50 publications

(37 citation statements)

References 59 publications

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“…The roles and mechanisms of miR-142-3p in NPC metastasis remain undefined. We demonstrated that miR-142-3p functioned as a suppressor in NPC metastasis, which is consistent with the inhibitory effects of miR-142-3p in other cancer types [31][32][33]. However, previous study showed a conversely promoted phenotype of miR-142-3p in NPC cell proliferation [34].…”

Section: Discussionsupporting

confidence: 87%

EZH2-DNMT1-mediated epigenetic silencing of miR-142-3p promotes metastasis through targeting ZEB2 in nasopharyngeal carcinoma

Wen

et al. 2018

Cell Death Differ

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Human nasopharyngeal carcinoma (NPC) has the highest metastatic rate in head and neck. However, the mechanisms underlying NPC metastasis remain unclear. Here using propensity-score-matched miRNA microarray analysis, miR-142-3p is identified to be the most correlated with distant-metastasis-free survival and downregulated in paraffin-embedded NPC with distant metastasis, which is validated in both internal cohort and external GEO dataset from Canada. miR-142 locus hypermethylation was observed and found to be associated with miR-142-3p downregulation in metastatic NPC. Furthermore, miR-142-3p was epigenetically silenced by EZH2-recruited DNMT1 and suppressed NPC cell metastasis and EMT. Intersecting PCR array gene profiling with bioinformatic prediction, we identify ZEB2 as a direct and functional target of miR-142-3p in NPC. Reversal of miR-142-3p silencing efficiently suppresses NPC cell invasion and metastasis. Moreover, epigenetic miR-142 hypermethylation is correlated with unfavorable prognosis in both training and validation cohorts. This study identifies miR-142-3p as a key suppressive regulator in NPC metastasis and reveals a DNMT1-mediated epigenetic mechanism for miR-142-3p silencing, providing a potential prognostic marker and therapeutic target to combat NPC metastasis.

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Section: Discussionsupporting

confidence: 87%

EZH2-DNMT1-mediated epigenetic silencing of miR-142-3p promotes metastasis through targeting ZEB2 in nasopharyngeal carcinoma

Wen

et al. 2018

Cell Death Differ

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“…MicroRNAs are non-coding RNAs which participate in cellular activity by regulating target genes. Increasing number of studies have reported that microRNAs are frequently differentially expressed in numerous types of human cancer and play an important role in the progression and development of NSCLC ( Inamura and Ishikawa, 2016 ; Berrout et al, 2017 ; Chang et al, 2017 ; Zhang et al, 2017 ; Iqbal et al, 2018 ). Although microRNAs act only in the cell where they are synthesized, they can also influence the functions of neighboring cells or play a role in the tumor micro-environment by modulating the ECM state ( Rutnam et al, 2013 ).…”

Section: Resultsmentioning

confidence: 99%

Integrative Analysis of Membrane Proteome and MicroRNA Reveals Novel Lung Cancer Metastasis Biomarkers

et al. 2020

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“…In this study, we chose a rabbit extracellular TRPA1 antibody for several reasons: (1) this antibody has been well characterized by the vendor, demonstrating a high specificity against an epitope (NSTGIINETSDHSE) corresponding to amino acid residues 747 to 760 in the first extracellular loop of TRPA1 ( Figure 1a); (2) the specificity has been verified in TRPA1 knockout tissue; 38 and (3) it consistently detects TRPA1 expression by IHC or immunoblot from DRGs and from nonneuronal tissues. 19,[36][37][38]40,[53][54][55][56][57][58][59][60][61][62][63] We also tested the specificity of this antibody in the detection of TRPA1 expression. By immunoblot, the antibody revealed a clean band at $120 KDa as the target protein in the homogenates of the DRGs from adult rats, and preincubation with excess immunogenic peptide completely eliminated the band (Figure 1b).…”

Section: Trpa1 Is Expressed In Primary Sensory Neurons Sgcs and Scsmentioning

confidence: 99%

Satellite glial cells in sensory ganglia express functional transient receptor potential ankyrin 1 that is sensitized in neuropathic and inflammatory pain

et al. 2020

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Transient receptor potential ankyrin 1 (TRPA1) is well documented as an important molecule in pain hypersensitivity following inflammation and nerve injury and in many other cellular biological processes. Here, we show that TRPA1 is expressed not only by sensory neurons of the dorsal root ganglia (DRG) but also in their adjacent satellite glial cells (SGCs), as well as nonmyelinating Schwann cells. TRPA1 immunoreactivity is also detected in various cutaneous structures of sensory neuronal terminals, including small and large caliber cutaneous sensory fibers and endings. The SGC-expressed TRPA1 is functional. Like DRG neurons, dissociated SGCs exhibit a robust response to the TRPA1-selective agonist allyl isothiocyanate (AITC) by an increase of intracellular Ca2+ concentration ([Ca2+]i). These responses are abolished by the TRPA1 antagonist HC030031 and are absent in SGCs and neurons from global TRPA1 null mice. SGCs and neurons harvested from DRG proximal to painful tissue inflammation induced by plantar injection of complete Freund’s adjuvant show greater AITC-evoked elevation of [Ca2+]i and slower recovery compared to sham controls. Similar TRPA1 sensitization occurs in both SGCs and neurons during neuropathic pain induced by spared nerve injury. Together, these results show that functional TRPA1 is expressed by sensory ganglia SGCs, and TRPA1 function in SGCs is enhanced after both peripheral inflammation and nerve injury, and suggest that TRPA1 in SGCs may contribute to inflammatory and neuropathic pain.

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TRPA1–FGFR2 binding event is a regulatory oncogenic driver modulated by miRNA-142-3p

Cited by 50 publications

References 59 publications

EZH2-DNMT1-mediated epigenetic silencing of miR-142-3p promotes metastasis through targeting ZEB2 in nasopharyngeal carcinoma

EZH2-DNMT1-mediated epigenetic silencing of miR-142-3p promotes metastasis through targeting ZEB2 in nasopharyngeal carcinoma

Integrative Analysis of Membrane Proteome and MicroRNA Reveals Novel Lung Cancer Metastasis Biomarkers

Satellite glial cells in sensory ganglia express functional transient receptor potential ankyrin 1 that is sensitized in neuropathic and inflammatory pain

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