SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2892044667> ?p ?o ?g. }

Showing items 1 to 100 of ±173 with 100 items per page.

W2892044667 abstract "Oligodendrocytes are highly vulnerable to glutamate excitotoxicity, a central mechanism involved in tissue damage in Multiple Sclerosis (MS). Sustained activation of AMPA receptors in rat oligodendrocytes induces cytosolic calcium overload, mitochondrial depolarization, increase of reactive oxygen species, and activation of intracelular pathways resulting in apoptotic cell death. Although many signals driven by excitotoxicity have been identified, some of the key players are still under investigation. Casein kinase 2 (CK2) is a serine/threonine kinase, constitutively expressed in all eukaryotic tissues, involved in cell proliferation, malignant transformation and apoptosis. In this study, we identify CK2 as a critical regulator of oligodendrocytic death pathways and elucidate its role as a signal inductor following excitotoxic insults. We provide evidence that CK2 activity is up-regulated in AMPA-treated oligodendrocytes and CK2 inhibition significantly diminished AMPA receptor-induced oligodendroglial death. In addition, we analyzed mitogen-activated protein kinase (MAPK) signaling after excitotoxic insult. We observed that AMPA receptor activation induced a rapid increase in c-Jun N-terminal kinase (JNK) and p38 phosphorylation that was reduced after CK2 inhibition. Moreover, blocking their phosphorylation, we enhanced oligodendrocyte survival after excitotoxic insult. Finally, we observed that the tumor suppressor p53 is activated during AMPA receptor-induced cell death and, interestingly, down-regulated by JNK or CK2 inhibition. Together, these data indicate that the increase in CK2 activity induced by excitotoxic insults regulates MAPKs, triggers p53 activation and mediates subsequent oligodendroglial loss. Therefore, targeting CK2 may be a useful strategy to prevent oligodendrocyte death in MS and other diseases involving central nervous system (CNS) white matter." @default.
W2892044667 created "2018-09-27" @default.
W2892044667 creator A5003131263 @default.
W2892044667 creator A5010284249 @default.
W2892044667 creator A5024944246 @default.
W2892044667 creator A5028302062 @default.
W2892044667 creator A5049443739 @default.
W2892044667 creator A5059651839 @default.
W2892044667 creator A5067478190 @default.
W2892044667 creator A5072085025 @default.
W2892044667 creator A5089159607 @default.
W2892044667 creator A5090360737 @default.
W2892044667 date "2018-09-13" @default.
W2892044667 modified "2023-10-18" @default.
W2892044667 title "Inhibition of Casein Kinase 2 Protects Oligodendrocytes From Excitotoxicity by Attenuating JNK/p53 Signaling Cascade" @default.
W2892044667 cites W1521392240 @default.
W2892044667 cites W1526564054 @default.
W2892044667 cites W1527012882 @default.
W2892044667 cites W1602259950 @default.
W2892044667 cites W1861665996 @default.
W2892044667 cites W1890581590 @default.
W2892044667 cites W1891032831 @default.
W2892044667 cites W1920097203 @default.
W2892044667 cites W1966669560 @default.
W2892044667 cites W1971748792 @default.
W2892044667 cites W1972673753 @default.
W2892044667 cites W1977362522 @default.
W2892044667 cites W1979286651 @default.
W2892044667 cites W1984156662 @default.
W2892044667 cites W1992191761 @default.
W2892044667 cites W1993246806 @default.
W2892044667 cites W1995773170 @default.
W2892044667 cites W1996547558 @default.
W2892044667 cites W1996745436 @default.
W2892044667 cites W1997003323 @default.
W2892044667 cites W2002091021 @default.
W2892044667 cites W2004204421 @default.
W2892044667 cites W2005894923 @default.
W2892044667 cites W2005922151 @default.
W2892044667 cites W2008933923 @default.
W2892044667 cites W2009398322 @default.
W2892044667 cites W2012116432 @default.
W2892044667 cites W2013551056 @default.
W2892044667 cites W2015178996 @default.
W2892044667 cites W2016575029 @default.
W2892044667 cites W2019702139 @default.
W2892044667 cites W2021152062 @default.
W2892044667 cites W2021800980 @default.
W2892044667 cites W2028341008 @default.
W2892044667 cites W2032603938 @default.
W2892044667 cites W2053440290 @default.
W2892044667 cites W2053504861 @default.
W2892044667 cites W2059021281 @default.
W2892044667 cites W2059994807 @default.
W2892044667 cites W2060295116 @default.
W2892044667 cites W2061823746 @default.
W2892044667 cites W2062793260 @default.
W2892044667 cites W2063953032 @default.
W2892044667 cites W2064734933 @default.
W2892044667 cites W2070330288 @default.
W2892044667 cites W2070749396 @default.
W2892044667 cites W2072926617 @default.
W2892044667 cites W2075655729 @default.
W2892044667 cites W2077236132 @default.
W2892044667 cites W2081504343 @default.
W2892044667 cites W2084963309 @default.
W2892044667 cites W2087527433 @default.
W2892044667 cites W2090548106 @default.
W2892044667 cites W2090684431 @default.
W2892044667 cites W2093608868 @default.
W2892044667 cites W2093611899 @default.
W2892044667 cites W2095052060 @default.
W2892044667 cites W2103615857 @default.
W2892044667 cites W2107495112 @default.
W2892044667 cites W2108653118 @default.
W2892044667 cites W2113106822 @default.
W2892044667 cites W2117275311 @default.
W2892044667 cites W2120194551 @default.
W2892044667 cites W2123618943 @default.
W2892044667 cites W2126365703 @default.
W2892044667 cites W2129881449 @default.
W2892044667 cites W2132296918 @default.
W2892044667 cites W2136607709 @default.
W2892044667 cites W2142098891 @default.
W2892044667 cites W2145324729 @default.
W2892044667 cites W2148073828 @default.
W2892044667 cites W2152351093 @default.
W2892044667 cites W2152635758 @default.
W2892044667 cites W2154025261 @default.
W2892044667 cites W2154274251 @default.
W2892044667 cites W2158707363 @default.
W2892044667 cites W2167264988 @default.
W2892044667 cites W2229426556 @default.
W2892044667 cites W2316145923 @default.
W2892044667 cites W2336719658 @default.
W2892044667 cites W2511362679 @default.
W2892044667 cites W2567439410 @default.
W2892044667 cites W2614085156 @default.
W2892044667 doi "https://doi.org/10.3389/fnmol.2018.00333" @default.
W2892044667 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6146035" @default.