FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2090500556> ?p ?o ?g. }

• W2090500556 endingPage "203" @default.
• W2090500556 startingPage "193" @default.
• W2090500556 abstract "The RAS (renin–angiotensin system) plays a role not only in the cardiovascular system, including blood pressure regulation, but also in the central nervous system. AngII (angiotensin II) binds two major receptors: the AT1 receptor (AngII type 1 receptor) and AT2 receptor (AngII type 2 receptor). It has been recognized that AT2 receptor activation not only opposes AT1 receptor actions, but also has unique effects beyond inhibitory cross-talk with AT1 receptor signalling. Novel pathways beyond the classical actions of RAS, the ACE (angiotensin-converting enzyme)/AngII/AT1 receptor axis, have been highlighted: the ACE2/Ang-(1–7) [angiotensin-(1–7)]/Mas receptor axis as a new opposing axis against the ACE/AngII/AT1 receptor axis, novel AngII-receptor-interacting proteins and various AngII-receptor-activation mechanisms including dimer formation. ATRAP (AT1-receptor-associated protein) and ATIP (AT2-receptor-interacting protein) are well-characterized AngII-receptor-associated proteins. These proteins could regulate the functions of AngII receptors and thereby influence various pathophysiological states. Moreover, the possible cross-talk between PPAR (peroxisome-proliferator-activated receptor)-γ and AngII receptor subtypes is an intriguing issue to be addressed in order to understand the roles of RAS in the metabolic syndrome, and interestingly some ARBs (AT1-receptor blockers) have been reported to have an AT1-receptor-blocking action with a partial PPAR-γ agonistic effect. These emerging concepts concerning the regulation of AngII receptors are discussed in the present review." @default.
• W2090500556 created "2016-06-24" @default.
• W2090500556 creator A5001563356 @default.
• W2090500556 creator A5011935809 @default.
• W2090500556 creator A5012868995 @default.
• W2090500556 date "2012-04-20" @default.
• W2090500556 modified "2023-09-23" @default.
• W2090500556 title "Regulation of angiotensin II receptors beyond the classical pathway" @default.
• W2090500556 cites W1512110535 @default.
• W2090500556 cites W1520957183 @default.
• W2090500556 cites W1559798894 @default.
• W2090500556 cites W1563194902 @default.
• W2090500556 cites W1594358562 @default.
• W2090500556 cites W1975454274 @default.
• W2090500556 cites W1978387124 @default.
• W2090500556 cites W1979349275 @default.
• W2090500556 cites W1982516779 @default.
• W2090500556 cites W1984520586 @default.
• W2090500556 cites W1991461625 @default.
• W2090500556 cites W1994105580 @default.
• W2090500556 cites W2007370298 @default.
• W2090500556 cites W2007861988 @default.
• W2090500556 cites W2008029981 @default.
• W2090500556 cites W2008048680 @default.
• W2090500556 cites W2011974109 @default.
• W2090500556 cites W2016656766 @default.
• W2090500556 cites W2018263437 @default.
• W2090500556 cites W2018545707 @default.
• W2090500556 cites W2024487267 @default.
• W2090500556 cites W2029022504 @default.
• W2090500556 cites W2032486084 @default.
• W2090500556 cites W2033942832 @default.
• W2090500556 cites W2033999361 @default.
• W2090500556 cites W2034781152 @default.
• W2090500556 cites W2035591978 @default.
• W2090500556 cites W2036894466 @default.
• W2090500556 cites W2039912643 @default.
• W2090500556 cites W2048748448 @default.
• W2090500556 cites W2050584514 @default.
• W2090500556 cites W2053127822 @default.
• W2090500556 cites W2054409489 @default.
• W2090500556 cites W2057076603 @default.
• W2090500556 cites W2057441702 @default.
• W2090500556 cites W2057989030 @default.
• W2090500556 cites W2064068272 @default.
• W2090500556 cites W2064650334 @default.
• W2090500556 cites W2067142583 @default.
• W2090500556 cites W2067802991 @default.
• W2090500556 cites W2070374666 @default.
• W2090500556 cites W2071497437 @default.
• W2090500556 cites W2072477280 @default.
• W2090500556 cites W2077553640 @default.
• W2090500556 cites W2105969731 @default.
• W2090500556 cites W2106122924 @default.
• W2090500556 cites W2112903359 @default.
• W2090500556 cites W2115787462 @default.
• W2090500556 cites W2116593104 @default.
• W2090500556 cites W2117645517 @default.
• W2090500556 cites W2117854326 @default.
• W2090500556 cites W2119678013 @default.
• W2090500556 cites W2121985419 @default.
• W2090500556 cites W2122256980 @default.
• W2090500556 cites W2127432761 @default.
• W2090500556 cites W2129697991 @default.
• W2090500556 cites W2134600182 @default.
• W2090500556 cites W2135733191 @default.
• W2090500556 cites W2136117114 @default.
• W2090500556 cites W2136566187 @default.
• W2090500556 cites W2138268766 @default.
• W2090500556 cites W2140137540 @default.
• W2090500556 cites W2142617203 @default.
• W2090500556 cites W2146490898 @default.
• W2090500556 cites W2148874697 @default.
• W2090500556 cites W2152975936 @default.
• W2090500556 cites W2154660221 @default.
• W2090500556 cites W2159245100 @default.
• W2090500556 cites W2159561716 @default.
• W2090500556 cites W2161097285 @default.
• W2090500556 cites W2163628953 @default.
• W2090500556 cites W2165954538 @default.
• W2090500556 cites W2169623875 @default.
• W2090500556 cites W2171172775 @default.
• W2090500556 cites W2226695198 @default.
• W2090500556 cites W2329179820 @default.
• W2090500556 cites W2335117204 @default.
• W2090500556 cites W4252397535 @default.
• W2090500556 doi "https://doi.org/10.1042/cs20110677" @default.
• W2090500556 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/22548405" @default.
• W2090500556 hasPublicationYear "2012" @default.
• W2090500556 type Work @default.
• W2090500556 sameAs 2090500556 @default.
• W2090500556 citedByCount "82" @default.
• W2090500556 countsByYear W20905005562012 @default.
• W2090500556 countsByYear W20905005562013 @default.
• W2090500556 countsByYear W20905005562014 @default.
• W2090500556 countsByYear W20905005562015 @default.
• W2090500556 countsByYear W20905005562016 @default.
• W2090500556 countsByYear W20905005562017 @default.

• next