FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2895826492> ?p ?o ?g. }

• W2895826492 endingPage "359" @default.
• W2895826492 startingPage "354" @default.
• W2895826492 abstract "Nicotinamide adenine dinucleotide (NAD+) is a co-substrate for several enzymes, including the sirtuin family of NAD+-dependent protein deacylases. Beneficial effects of increased NAD+ levels and sirtuin activation on mitochondrial homeostasis, organismal metabolism and lifespan have been established across species. Here we show that α-amino-β-carboxymuconate-e-semialdehyde decarboxylase (ACMSD), the enzyme that limits spontaneous cyclization of α-amino-β-carboxymuconate-e-semialdehyde in the de novo NAD+ synthesis pathway, controls cellular NAD+ levels via an evolutionarily conserved mechanism in Caenorhabditis elegans and mouse. Genetic and pharmacological inhibition of ACMSD boosts de novo NAD+ synthesis and sirtuin 1 activity, ultimately enhancing mitochondrial function. We also characterize two potent and selective inhibitors of ACMSD. Because expression of ACMSD is largely restricted to kidney and liver, these inhibitors may have therapeutic potential for protection of these tissues from injury. In summary, we identify ACMSD as a key modulator of cellular NAD+ levels, sirtuin activity and mitochondrial homeostasis in kidney and liver." @default.
• W2895826492 created "2018-10-26" @default.
• W2895826492 creator A5003154600 @default.
• W2895826492 creator A5004089526 @default.
• W2895826492 creator A5015359260 @default.
• W2895826492 creator A5018846000 @default.
• W2895826492 creator A5019819875 @default.
• W2895826492 creator A5028737784 @default.
• W2895826492 creator A5033554852 @default.
• W2895826492 creator A5045044750 @default.
• W2895826492 creator A5045698002 @default.
• W2895826492 creator A5045702168 @default.
• W2895826492 creator A5051530653 @default.
• W2895826492 creator A5063038555 @default.
• W2895826492 creator A5068338674 @default.
• W2895826492 creator A5068393615 @default.
• W2895826492 creator A5068717424 @default.
• W2895826492 creator A5077352717 @default.
• W2895826492 creator A5077405324 @default.
• W2895826492 creator A5083066932 @default.
• W2895826492 creator A5088404150 @default.
• W2895826492 date "2018-10-24" @default.
• W2895826492 modified "2023-10-16" @default.
• W2895826492 title "De novo NAD+ synthesis enhances mitochondrial function and improves health" @default.
• W2895826492 cites W1571431689 @default.
• W2895826492 cites W1656781980 @default.
• W2895826492 cites W1877188956 @default.
• W2895826492 cites W1972660602 @default.
• W2895826492 cites W1975144545 @default.
• W2895826492 cites W1977244638 @default.
• W2895826492 cites W1987240473 @default.
• W2895826492 cites W1989108323 @default.
• W2895826492 cites W2007107430 @default.
• W2895826492 cites W2012034410 @default.
• W2895826492 cites W2012043504 @default.
• W2895826492 cites W2015377162 @default.
• W2895826492 cites W2019240387 @default.
• W2895826492 cites W2028178274 @default.
• W2895826492 cites W2032022203 @default.
• W2895826492 cites W2032385561 @default.
• W2895826492 cites W2037047673 @default.
• W2895826492 cites W2053124968 @default.
• W2895826492 cites W2072718771 @default.
• W2895826492 cites W2074974899 @default.
• W2895826492 cites W2086066803 @default.
• W2895826492 cites W2088385225 @default.
• W2895826492 cites W2093048027 @default.
• W2895826492 cites W2111684219 @default.
• W2895826492 cites W2129550243 @default.
• W2895826492 cites W2143015660 @default.
• W2895826492 cites W2144600435 @default.
• W2895826492 cites W2146884956 @default.
• W2895826492 cites W2154877445 @default.
• W2895826492 cites W2164155587 @default.
• W2895826492 cites W2239653845 @default.
• W2895826492 cites W2298455799 @default.
• W2895826492 cites W2305670323 @default.
• W2895826492 cites W2406866966 @default.
• W2895826492 cites W2470982690 @default.
• W2895826492 cites W2516495404 @default.
• W2895826492 cites W2521759723 @default.
• W2895826492 cites W2527724013 @default.
• W2895826492 cites W2617221282 @default.
• W2895826492 cites W2743027547 @default.
• W2895826492 cites W2745226153 @default.
• W2895826492 cites W2782698292 @default.
• W2895826492 cites W2800314655 @default.
• W2895826492 cites W4255535345 @default.
• W2895826492 doi "https://doi.org/10.1038/s41586-018-0645-6" @default.
• W2895826492 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6448761" @default.
• W2895826492 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30356218" @default.
• W2895826492 hasPublicationYear "2018" @default.
• W2895826492 type Work @default.
• W2895826492 sameAs 2895826492 @default.
• W2895826492 citedByCount "267" @default.
• W2895826492 countsByYear W28958264922018 @default.
• W2895826492 countsByYear W28958264922019 @default.
• W2895826492 countsByYear W28958264922020 @default.
• W2895826492 countsByYear W28958264922021 @default.
• W2895826492 countsByYear W28958264922022 @default.
• W2895826492 countsByYear W28958264922023 @default.
• W2895826492 crossrefType "journal-article" @default.
• W2895826492 hasAuthorship W2895826492A5003154600 @default.
• W2895826492 hasAuthorship W2895826492A5004089526 @default.
• W2895826492 hasAuthorship W2895826492A5015359260 @default.
• W2895826492 hasAuthorship W2895826492A5018846000 @default.
• W2895826492 hasAuthorship W2895826492A5019819875 @default.
• W2895826492 hasAuthorship W2895826492A5028737784 @default.
• W2895826492 hasAuthorship W2895826492A5033554852 @default.
• W2895826492 hasAuthorship W2895826492A5045044750 @default.
• W2895826492 hasAuthorship W2895826492A5045698002 @default.
• W2895826492 hasAuthorship W2895826492A5045702168 @default.
• W2895826492 hasAuthorship W2895826492A5051530653 @default.
• W2895826492 hasAuthorship W2895826492A5063038555 @default.
• W2895826492 hasAuthorship W2895826492A5068338674 @default.
• W2895826492 hasAuthorship W2895826492A5068393615 @default.
• W2895826492 hasAuthorship W2895826492A5068717424 @default.
• W2895826492 hasAuthorship W2895826492A5077352717 @default.

• next