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2 research outputs found

Degradation of high affinity HuD targets releases Kv1.1 mRNA from miR-129 repression by mTORC1

Author: Aakalu
Abel
Albig
Ando
Antic
Bartel
Blichenberg
Bliss
Bolognani
Bolognani
Bolognani
Bolognani
Bolognani
Brew
Cajigas
Chen
Chun Jung Chen
Costa-Mattioli
Davis
Deschênes-Furry
Fabian
Filipowicz
Fukao
Geiger
George
Golding
Grimson
Grundhoff
Hoeffer
Hopkins
Kathleen Nguyen
Kim
Kim
Kimberly F. Raab-Graham
Klann
Konecna
Kosik
Kundu
Kuwano
Landgraf
Luisa P. Cacheaux
Ma
Martin
Meisner
Metz
Miska
Monaghan
Natasha M. Sosanya
Nora I. Perrone-Bizzozero
Origanti
Pascale
Peggy P.C. Huang
Pfaffl
Quinlan
Raab-Graham
Richter
Ronesi
Sahin
Schechter
Schratt
Sharma
Smart
Southan
Srikantan
Storm
Tanouye
Tiffany
Tiruchinapalli
Turrigiano
Vatolin
Volk
Wang
Wells
Williams
Wu
Xue
Zeng
Zerr
Zhang
Publication venue: 'Rockefeller University Press'
Publication date: 01/01/2013
Field of study

Little is known about how a neuron undergoes site-specific changes in intrinsic excitability during neuronal activity. We provide evidence for a novel mechanism for mTORC1 kinase–dependent translational regulation of the voltage-gated potassium channel Kv1.1 messenger RNA (mRNA). We identified a microRNA, miR-129, that repressed Kv1.1 mRNA translation when mTORC1 was active. When mTORC1 was inactive, we found that the RNA-binding protein, HuD, bound to Kv1.1 mRNA and promoted its translation. Unexpectedly, inhibition of mTORC1 activity did not alter levels of miR-129 and HuD to favor binding to Kv1.1 mRNA. However, reduced mTORC1 signaling caused the degradation of high affinity HuD target mRNAs, freeing HuD to bind Kv1.1 mRNA. Hence, mTORC1 activity regulation of mRNA stability and high affinity HuD-target mRNA degradation mediates the bidirectional expression of dendritic Kv1.1 ion channels

Crossref

PubMed Central

Texas A&M Repository

Involvement of brain-derived neurotrophic factor (BDNF) in chronic intermittent stress-induced enhanced mechanical allodynia in a rat model of burn pain

Author: Bopaiah P. Cheppudira
Natasha M. Sosanya
Robert J. Christy
Stephen L. Crimmins
Thomas H. Garza
Winfred Stacey
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/04/2019
Field of study

Abstract Background Reports show that stressful events before injury exacerbates post-injury pain. The mechanism underlying stress-induced heightened thermal pain is unclear. Here, we examined the effects of chronic intermittent stress (CIS) on nociceptive behaviors and brain-derived nerve growth factor (BDNF) system in the prefrontal cortex (PFC) and hypothalamus of rats with and without thermal injury. Results Unstressed rats showed transient mechanical allodynia during stress exposure. Stressed rats with thermal injury displayed persistent exacerbated mechanical allodynia (P < 0.001). Increased expression of BDNF mRNA in the PFC (P < 0.05), and elevated TrkB and p-TrkB (P < 0.05) protein levels in the hypothalamus were observed in stressed rats with thermal injury but not in stressed or thermally injured rats alone. Furthermore, administration of CTX-B significantly reduced stress-induced exacerbated mechanical allodynia in thermally injured rats (P < 0.001). Conclusion These results indicate that BDNF-TrkB signaling in PFC and hypothalamus contributes to CIS-induced exacerbated mechanical allodynia in thermal injury state

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