Vittorio De Santis scite author profile

HighlightsROS levels assessed in peripheral and central sensory neurons following paclitaxel.Increased ROS levels seen in non-peptidergic neurons prior to paclitaxel-induced pain.Elevated ROS levels in spinal neurons, but not microglia/astrocytes, after paclitaxel.Assayed activity of main antioxidant enzymes during paclitaxel-evoked pain timecourse.Inadequate antioxidant response suggests elevated ROS sustains paclitaxel-evoked pain.

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TAB1-Induced Autoactivation of p38α Mitogen-Activated Protein Kinase Is Crucially Dependent on Threonine 185

Thapa

Nichols

Bassi

et al. 2018

Molecular and Cellular Biology

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ABSTRACTp38α mitogen-activated protein kinase is essential to cellular homeostasis. Two principal mechanisms to activate p38α exist. The first relies on dedicated dual-specificity kinases such as mitogen-activated protein kinase kinase (MAP2K) 3 (MKK3) or 6 (MKK6), which activate p38α by phosphorylating Thr180 and Tyr182 within the activation segment. The second is by autophosphorylation of Thr180 and Tyr182 in cis, mediated by p38α binding the scaffold protein TAB1. The second mechanism occurs during myocardial ischemia, where it aggravates myocardial infarction. Based on the crystal structure of the p38α-TAB1 complex we replaced threonine 185 of p38α with glycine (T185G) to prevent an intramolecular hydrogen bond with Asp150 from being formed. This mutation did not interfere with TAB1 binding to p38α. However, it disrupted the consequent long-range effect of this binding event on the distal activation segment, releasing the constraint on Thr180 that oriented its hydroxyl for phosphotransfer. Based on assays performed in vitro and in vivo, the autoactivation of p38α(T185G) was disabled, while its ability to be activated by upstream MAP2Ks and to phosphorylate downstream substrates remained intact. Furthermore, myocardial cells expressing p38α(T185G) were resistant to injury. These findings reveal a mechanism to selectively disable p38α autoactivation and its consequences, which may ultimately circumvent the toxicity associated with strategies that inhibit p38α kinase activity under all circumstances, such as with ATP-competitive inhibitors.

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Influence of agonist induced internalization on [³H]Ro15‐4513 binding—an application to imaging fluctuations in endogenous GABA with positron emission tomography

Quelch

Santis²,

Strege

et al. 2014

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