SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W3161796677> ?p ?o ?g. }

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

W3161796677 endingPage "106013" @default.
W3161796677 startingPage "106013" @default.
W3161796677 abstract "The NLR family pyrin domain containing 3 (NLRP3) inflammasome is responsible for the sensation of various pathogenic and non-pathogenic damage signals and has a vital role in neuroinflammation and neural diseases. Various stimuli, such as microbial infection, misfolded protein aggregates, and aberrant deposition of proteins can induce NLRP3 inflammasome in neural cells. Once triggered, the NLRP3 inflammasome leads to the activation of caspase-1, which in turn activates inflammatory cytokines, such as interleukin-1β and interleukin -18, and induces pyroptotic cell death. Mitochondria are critically involved in diverse cellular processes and are involved in regulating cellular redox status, calcium levels, inflammasome activation, and cell death. Mitochondrial dysfunction and subsequent accumulation of mitochondrial reactive oxygen species, mitochondrial deoxyribonucleic acid, and other mitochondria-associated proteins and lipids play vital roles in the instigation of the NLRP3 inflammasome. In addition, the processes of mitochondrial dynamics, such as fission and fusion, are essential in the maintenance of mitochondrial integrity and their imbalance also promotes NLRP3 inflammasome activation. In this connection, mitophagy-mediated maintenance of mitochondrial homeostasis restricts NLRP3 inflammasome hyperactivation and its consequences in various neurological disorders. Hence, mitophagy can be exploited as a potential strategy to target damaged mitochondria induced NLRP3 inflammasome activation and its lethal consequences. Therefore, the identification of novel mitophagy modulators has promising therapeutic potential for NLRP3 inflammasome-associated neuronal diseases." @default.
W3161796677 created "2021-05-24" @default.
W3161796677 creator A5002224920 @default.
W3161796677 creator A5002697297 @default.
W3161796677 creator A5013562692 @default.
W3161796677 creator A5017183210 @default.
W3161796677 creator A5035317652 @default.
W3161796677 creator A5035677903 @default.
W3161796677 creator A5040431431 @default.
W3161796677 creator A5043450835 @default.
W3161796677 creator A5054304436 @default.
W3161796677 creator A5065757572 @default.
W3161796677 creator A5084019473 @default.
W3161796677 date "2021-07-01" @default.
W3161796677 modified "2023-10-11" @default.
W3161796677 title "Mitochondrial dysfunction as a driver of NLRP3 inflammasome activation and its modulation through mitophagy for potential therapeutics" @default.
W3161796677 cites W1974744480 @default.
W3161796677 cites W1976921001 @default.
W3161796677 cites W1985538633 @default.
W3161796677 cites W1989026904 @default.
W3161796677 cites W1999224782 @default.
W3161796677 cites W2001946532 @default.
W3161796677 cites W2002394315 @default.
W3161796677 cites W2010508038 @default.
W3161796677 cites W2018563185 @default.
W3161796677 cites W2025673880 @default.
W3161796677 cites W2037600884 @default.
W3161796677 cites W2038976751 @default.
W3161796677 cites W2044911918 @default.
W3161796677 cites W2049016912 @default.
W3161796677 cites W2067406680 @default.
W3161796677 cites W2090711760 @default.
W3161796677 cites W2092817697 @default.
W3161796677 cites W2113010696 @default.
W3161796677 cites W2131007152 @default.
W3161796677 cites W2155738620 @default.
W3161796677 cites W2157352436 @default.
W3161796677 cites W2162633290 @default.
W3161796677 cites W2166682453 @default.
W3161796677 cites W2176443454 @default.
W3161796677 cites W2209731801 @default.
W3161796677 cites W2210680772 @default.
W3161796677 cites W2254807163 @default.
W3161796677 cites W2275879522 @default.
W3161796677 cites W2290088765 @default.
W3161796677 cites W2415916782 @default.
W3161796677 cites W2460178156 @default.
W3161796677 cites W2462773201 @default.
W3161796677 cites W2492083962 @default.
W3161796677 cites W2510531327 @default.
W3161796677 cites W2520186370 @default.
W3161796677 cites W2522054313 @default.
W3161796677 cites W2616329870 @default.
W3161796677 cites W2620896337 @default.
W3161796677 cites W2732648784 @default.
W3161796677 cites W2761027295 @default.
W3161796677 cites W2761217496 @default.
W3161796677 cites W2775627464 @default.
W3161796677 cites W2796818595 @default.
W3161796677 cites W2884556905 @default.
W3161796677 cites W2890204725 @default.
W3161796677 cites W2891015697 @default.
W3161796677 cites W2903402969 @default.
W3161796677 cites W2903992857 @default.
W3161796677 cites W2904217430 @default.
W3161796677 cites W2905213246 @default.
W3161796677 cites W2907424910 @default.
W3161796677 cites W2907636734 @default.
W3161796677 cites W2909458901 @default.
W3161796677 cites W2911549495 @default.
W3161796677 cites W2913910166 @default.
W3161796677 cites W2918118732 @default.
W3161796677 cites W2923199598 @default.
W3161796677 cites W2943293743 @default.
W3161796677 cites W2948231834 @default.
W3161796677 cites W2952863642 @default.
W3161796677 cites W2954558590 @default.
W3161796677 cites W2964186349 @default.
W3161796677 cites W2964527509 @default.
W3161796677 cites W2966499869 @default.
W3161796677 cites W2967134419 @default.
W3161796677 cites W2973473061 @default.
W3161796677 cites W2974579689 @default.
W3161796677 cites W2978810474 @default.
W3161796677 cites W2979288514 @default.
W3161796677 cites W2995758444 @default.
W3161796677 cites W2998324388 @default.
W3161796677 cites W3004905553 @default.
W3161796677 cites W3011802680 @default.
W3161796677 cites W3017735985 @default.
W3161796677 cites W3017989357 @default.
W3161796677 cites W3033829306 @default.
W3161796677 cites W3048762992 @default.
W3161796677 cites W3088021016 @default.
W3161796677 cites W4211217520 @default.
W3161796677 doi "https://doi.org/10.1016/j.biocel.2021.106013" @default.
W3161796677 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/34022434" @default.
W3161796677 hasPublicationYear "2021" @default.