FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2104828162> ?p ?o ?g. }

• W2104828162 endingPage "2757" @default.
• W2104828162 startingPage "2747" @default.
• W2104828162 abstract "The second messengers cAMP and cGMP can be degraded by specific members of the phosphodiesterase superfamily or by active efflux transporters, namely the multidrug resistance-associated proteins (MRPs) MRP4 and MRP5. To determine the role of MRP4 and MRP5 in cell signaling, we studied arterial SMCs, in which the effects of cyclic nucleotide levels on SMC proliferation have been well established. We found that MRP4, but not MRP5, was upregulated during proliferation of isolated human coronary artery SMCs and following injury of rat carotid arteries in vivo. MRP4 inhibition significantly increased intracellular cAMP and cGMP levels and was sufficient to block proliferation and to prevent neointimal growth in injured rat carotid arteries. The antiproliferative effect of MRP4 inhibition was related to PKA/CREB pathway activation. Here we provide what we believe to be the first evidence that MRP4 acts as an independent endogenous regulator of intracellular cyclic nucleotide levels and as a mediator of cAMP-dependent signal transduction to the nucleus. We also identify MRP4 inhibition as a potentially new way of preventing abnormal VSMC proliferation." @default.
• W2104828162 created "2016-06-24" @default.
• W2104828162 creator A5002624513 @default.
• W2104828162 creator A5008048278 @default.
• W2104828162 creator A5026564613 @default.
• W2104828162 creator A5029343789 @default.
• W2104828162 creator A5031426939 @default.
• W2104828162 creator A5051146510 @default.
• W2104828162 creator A5055750095 @default.
• W2104828162 creator A5067372053 @default.
• W2104828162 creator A5068357169 @default.
• W2104828162 creator A5070456505 @default.
• W2104828162 creator A5072560625 @default.
• W2104828162 creator A5077621721 @default.
• W2104828162 date "2008-08-01" @default.
• W2104828162 modified "2023-10-10" @default.
• W2104828162 title "Multidrug resistance-associated protein 4 regulates cAMP-dependent signaling pathways and controls human and rat SMC proliferation" @default.
• W2104828162 cites W1488600025 @default.
• W2104828162 cites W1583251544 @default.
• W2104828162 cites W1834533906 @default.
• W2104828162 cites W1965781254 @default.
• W2104828162 cites W1966431705 @default.
• W2104828162 cites W1968745182 @default.
• W2104828162 cites W1971748110 @default.
• W2104828162 cites W1978545009 @default.
• W2104828162 cites W1982482091 @default.
• W2104828162 cites W1986602912 @default.
• W2104828162 cites W1987430295 @default.
• W2104828162 cites W1997566004 @default.
• W2104828162 cites W1997819209 @default.
• W2104828162 cites W1999970975 @default.
• W2104828162 cites W2013654757 @default.
• W2104828162 cites W2016305001 @default.
• W2104828162 cites W2023191701 @default.
• W2104828162 cites W2023589885 @default.
• W2104828162 cites W2026574273 @default.
• W2104828162 cites W2029299795 @default.
• W2104828162 cites W2032408491 @default.
• W2104828162 cites W2035773315 @default.
• W2104828162 cites W2042674837 @default.
• W2104828162 cites W2063716341 @default.
• W2104828162 cites W2065965392 @default.
• W2104828162 cites W2083524015 @default.
• W2104828162 cites W2093935222 @default.
• W2104828162 cites W2100808729 @default.
• W2104828162 cites W2102156351 @default.
• W2104828162 cites W2105297145 @default.
• W2104828162 cites W2106517675 @default.
• W2104828162 cites W2106762675 @default.
• W2104828162 cites W2107034951 @default.
• W2104828162 cites W2108660541 @default.
• W2104828162 cites W2108833026 @default.
• W2104828162 cites W2111567736 @default.
• W2104828162 cites W2112299788 @default.
• W2104828162 cites W2112720988 @default.
• W2104828162 cites W2114467087 @default.
• W2104828162 cites W2133553247 @default.
• W2104828162 cites W2134712306 @default.
• W2104828162 cites W2139864041 @default.
• W2104828162 cites W2139915912 @default.
• W2104828162 cites W2142030049 @default.
• W2104828162 cites W2149683055 @default.
• W2104828162 cites W2151593414 @default.
• W2104828162 cites W2151625463 @default.
• W2104828162 cites W2154271343 @default.
• W2104828162 cites W2156094398 @default.
• W2104828162 cites W2161789882 @default.
• W2104828162 cites W2163571423 @default.
• W2104828162 cites W2164514432 @default.
• W2104828162 cites W2165860016 @default.
• W2104828162 cites W2167652900 @default.
• W2104828162 cites W2171796334 @default.
• W2104828162 cites W2267941286 @default.
• W2104828162 cites W2339699486 @default.
• W2104828162 doi "https://doi.org/10.1172/jci35067" @default.
• W2104828162 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/2467383" @default.
• W2104828162 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/18636120" @default.
• W2104828162 hasPublicationYear "2008" @default.
• W2104828162 type Work @default.
• W2104828162 sameAs 2104828162 @default.
• W2104828162 citedByCount "112" @default.
• W2104828162 countsByYear W21048281622012 @default.
• W2104828162 countsByYear W21048281622013 @default.
• W2104828162 countsByYear W21048281622014 @default.
• W2104828162 countsByYear W21048281622015 @default.
• W2104828162 countsByYear W21048281622016 @default.
• W2104828162 countsByYear W21048281622017 @default.
• W2104828162 countsByYear W21048281622018 @default.
• W2104828162 countsByYear W21048281622019 @default.
• W2104828162 countsByYear W21048281622020 @default.
• W2104828162 countsByYear W21048281622021 @default.
• W2104828162 countsByYear W21048281622022 @default.
• W2104828162 countsByYear W21048281622023 @default.
• W2104828162 crossrefType "journal-article" @default.
• W2104828162 hasAuthorship W2104828162A5002624513 @default.
• W2104828162 hasAuthorship W2104828162A5008048278 @default.
• W2104828162 hasAuthorship W2104828162A5026564613 @default.
• W2104828162 hasAuthorship W2104828162A5029343789 @default.

• next