FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2014202408> ?p ?o ?g. }

• W2014202408 endingPage "465" @default.
• W2014202408 startingPage "457" @default.
• W2014202408 abstract "MTAP (5′-methylthioadenosine phosphorylase) catalyses the reversible phosphorolytic cleavage of methylthioadenosine leading to the production of methylthioribose-1-phosphate and adenine. Deficient MTAP activity has been correlated with human diseases including cirrhosis and hepatocellular carcinoma. In the present study we have investigated the regulation of MTAP by ROS (reactive oxygen species). The results of the present study support the inactivation of MTAP in the liver of bacterial LPS (lipopolysaccharide)-challenged mice as well as in HepG2 cells after exposure to t-butyl hydroperoxide. Reversible inactivation of purified MTAP by hydrogen peroxide results from a reduction of Vmax and involves the specific oxidation of Cys136 and Cys223 thiols to sulfenic acid that may be further stabilized to sulfenyl amide intermediates. Additionally, we found that Cys145 and Cys211 were disulfide bonded upon hydrogen peroxide exposure. However, this modification is not relevant to the mediation of the loss of MTAP activity as assessed by site-directed mutagenesis. Regulation of MTAP by ROS might participate in the redox regulation of the methionine catabolic pathway in the liver. Reduced MTA (5′-deoxy-5′-methylthioadenosine)-degrading activity may compensate for the deficient production of the precursor S-adenosylmethionine, allowing maintenance of intracellular MTA levels that may be critical to ensure cellular adaptation to physiopathological conditions such as inflammation." @default.
• W2014202408 created "2016-06-24" @default.
• W2014202408 creator A5002412589 @default.
• W2014202408 creator A5003710944 @default.
• W2014202408 creator A5006711564 @default.
• W2014202408 creator A5012981755 @default.
• W2014202408 creator A5015399536 @default.
• W2014202408 creator A5030912350 @default.
• W2014202408 creator A5040716806 @default.
• W2014202408 creator A5060637503 @default.
• W2014202408 creator A5070340774 @default.
• W2014202408 creator A5075567314 @default.
• W2014202408 creator A5076205150 @default.
• W2014202408 date "2008-03-27" @default.
• W2014202408 modified "2023-10-18" @default.
• W2014202408 title "Redox regulation of methylthioadenosine phosphorylase in liver cells: molecular mechanism and functional implications" @default.
• W2014202408 cites W111483988 @default.
• W2014202408 cites W1525948692 @default.
• W2014202408 cites W1536591983 @default.
• W2014202408 cites W1538862365 @default.
• W2014202408 cites W1567096247 @default.
• W2014202408 cites W1578809256 @default.
• W2014202408 cites W1603847643 @default.
• W2014202408 cites W192690905 @default.
• W2014202408 cites W1966510680 @default.
• W2014202408 cites W1976981858 @default.
• W2014202408 cites W1980382813 @default.
• W2014202408 cites W1981926367 @default.
• W2014202408 cites W1990754063 @default.
• W2014202408 cites W2001569378 @default.
• W2014202408 cites W2006087749 @default.
• W2014202408 cites W2006370393 @default.
• W2014202408 cites W2013533113 @default.
• W2014202408 cites W2015990290 @default.
• W2014202408 cites W2018404966 @default.
• W2014202408 cites W2029385390 @default.
• W2014202408 cites W2043712928 @default.
• W2014202408 cites W2044761859 @default.
• W2014202408 cites W2052464531 @default.
• W2014202408 cites W2053242176 @default.
• W2014202408 cites W2054191209 @default.
• W2014202408 cites W2065342373 @default.
• W2014202408 cites W2070454905 @default.
• W2014202408 cites W2072880784 @default.
• W2014202408 cites W2073133083 @default.
• W2014202408 cites W2080738906 @default.
• W2014202408 cites W2089713346 @default.
• W2014202408 cites W2099817964 @default.
• W2014202408 cites W2100837269 @default.
• W2014202408 cites W2109734459 @default.
• W2014202408 cites W2115861175 @default.
• W2014202408 cites W2129777487 @default.
• W2014202408 cites W2137234652 @default.
• W2014202408 cites W2138398218 @default.
• W2014202408 cites W2147993424 @default.
• W2014202408 cites W2155203442 @default.
• W2014202408 cites W2160661817 @default.
• W2014202408 cites W2328271770 @default.
• W2014202408 cites W2343090247 @default.
• W2014202408 cites W4230795754 @default.
• W2014202408 cites W4293247451 @default.
• W2014202408 cites W4294216491 @default.
• W2014202408 doi "https://doi.org/10.1042/bj20071569" @default.
• W2014202408 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/18237276" @default.
• W2014202408 hasPublicationYear "2008" @default.
• W2014202408 type Work @default.
• W2014202408 sameAs 2014202408 @default.
• W2014202408 citedByCount "15" @default.
• W2014202408 countsByYear W20142024082013 @default.
• W2014202408 countsByYear W20142024082015 @default.
• W2014202408 countsByYear W20142024082016 @default.
• W2014202408 countsByYear W20142024082018 @default.
• W2014202408 countsByYear W20142024082021 @default.
• W2014202408 crossrefType "journal-article" @default.
• W2014202408 hasAuthorship W2014202408A5002412589 @default.
• W2014202408 hasAuthorship W2014202408A5003710944 @default.
• W2014202408 hasAuthorship W2014202408A5006711564 @default.
• W2014202408 hasAuthorship W2014202408A5012981755 @default.
• W2014202408 hasAuthorship W2014202408A5015399536 @default.
• W2014202408 hasAuthorship W2014202408A5030912350 @default.
• W2014202408 hasAuthorship W2014202408A5040716806 @default.
• W2014202408 hasAuthorship W2014202408A5060637503 @default.
• W2014202408 hasAuthorship W2014202408A5070340774 @default.
• W2014202408 hasAuthorship W2014202408A5075567314 @default.
• W2014202408 hasAuthorship W2014202408A5076205150 @default.
• W2014202408 hasBestOaLocation W20142024082 @default.
• W2014202408 hasConcept C181199279 @default.
• W2014202408 hasConcept C185592680 @default.
• W2014202408 hasConcept C2779201268 @default.
• W2014202408 hasConcept C2780158455 @default.
• W2014202408 hasConcept C2780912031 @default.
• W2014202408 hasConcept C2909420578 @default.
• W2014202408 hasConcept C48349386 @default.
• W2014202408 hasConcept C515207424 @default.
• W2014202408 hasConcept C533411734 @default.
• W2014202408 hasConcept C55493867 @default.
• W2014202408 hasConcept C62231903 @default.
• W2014202408 hasConcept C79879829 @default.

• next