FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2018203142> ?p ?o ?g. }

• W2018203142 endingPage "135" @default.
• W2018203142 startingPage "126" @default.
• W2018203142 abstract "The components of the kinin system, including kinongens, kininogenases, and B(2) and B(1) receptors, are expressed and activated during inflammation. Here, we investigated the expression of the kinin B(2) receptor messenger RNA, kininogen and kallikrein immunoreactivity, and the ability of kinins to contract control and inflamed gallbladders in vitro.Human gallbladders, obtained from patients undergoing cholecystectomy either for acute cholecystitis secondary to gallstone disease or during elective gastro-entero-pancreatic surgery (controls), were processed for reverse-transcription polymerase chain reaction analysis, kallikrein and kininogen immunohistochemistry, binding studies, and in vitro contractility studies.Tissue expression of B(2) receptor messenger RNA and specific binding of [(3)H]-bradykinin increased significantly in acute cholecystitis compared to controls. Kallikrein immunoreactivity was detected in the epithelium and infiltrating leukocytes, whereas kininogen immunoreactivity in the lumen of blood vessels and interstitial space. Bradykinin contracted isolated strips of control and acute cholecystitis gallbladders. In acute cholecystitis tissue, efficacy of bradykinin was higher than that of control gallbladders and similar to that of cholecystokinin. The contraction induced by bradykinin was significantly attenuated by B(2) receptor antagonism but not by cyclooxygenase inhibition and B(1), muscarinic, or tachykinin receptor antagonism.All the components of the kinin system are expressed in the human gallbladder. Bradykinin is a powerful spasmogen via B(2) receptor activation in the normal and, especially, in the inflamed human gallbladder." @default.
• W2018203142 created "2016-06-24" @default.
• W2018203142 creator A5000033590 @default.
• W2018203142 creator A5010623196 @default.
• W2018203142 creator A5025492450 @default.
• W2018203142 creator A5037408048 @default.
• W2018203142 creator A5048500290 @default.
• W2018203142 creator A5051065694 @default.
• W2018203142 creator A5052154744 @default.
• W2018203142 creator A5054158772 @default.
• W2018203142 creator A5056582101 @default.
• W2018203142 creator A5058796557 @default.
• W2018203142 creator A5076928480 @default.
• W2018203142 creator A5082448644 @default.
• W2018203142 creator A5088345375 @default.
• W2018203142 creator A5091033546 @default.
• W2018203142 date "2003-07-01" @default.
• W2018203142 modified "2023-09-27" @default.
• W2018203142 title "Bradykinin B2 receptors mediate contraction in the normal and inflamed human gallbladder in vitro" @default.
• W2018203142 cites W1572581981 @default.
• W2018203142 cites W1764686129 @default.
• W2018203142 cites W1827292456 @default.
• W2018203142 cites W1838482528 @default.
• W2018203142 cites W1964557305 @default.
• W2018203142 cites W1969984674 @default.
• W2018203142 cites W1971129717 @default.
• W2018203142 cites W1974146850 @default.
• W2018203142 cites W1975952670 @default.
• W2018203142 cites W1977251642 @default.
• W2018203142 cites W1984792851 @default.
• W2018203142 cites W2003383149 @default.
• W2018203142 cites W2013696867 @default.
• W2018203142 cites W2022575798 @default.
• W2018203142 cites W2024372998 @default.
• W2018203142 cites W2026585127 @default.
• W2018203142 cites W2027529370 @default.
• W2018203142 cites W2035117251 @default.
• W2018203142 cites W2038851375 @default.
• W2018203142 cites W2050344595 @default.
• W2018203142 cites W2053725221 @default.
• W2018203142 cites W2059285296 @default.
• W2018203142 cites W2070014029 @default.
• W2018203142 cites W2070121322 @default.
• W2018203142 cites W2073557461 @default.
• W2018203142 cites W2076658540 @default.
• W2018203142 cites W2083347538 @default.
• W2018203142 cites W2088560413 @default.
• W2018203142 cites W2091303128 @default.
• W2018203142 cites W2091338000 @default.
• W2018203142 cites W2091588586 @default.
• W2018203142 cites W2093198207 @default.
• W2018203142 cites W2101979009 @default.
• W2018203142 cites W2128635872 @default.
• W2018203142 cites W2131040260 @default.
• W2018203142 cites W2141455178 @default.
• W2018203142 cites W214850758 @default.
• W2018203142 cites W2167078616 @default.
• W2018203142 cites W2262763314 @default.
• W2018203142 cites W2406024938 @default.
• W2018203142 cites W2408554416 @default.
• W2018203142 cites W2416661247 @default.
• W2018203142 cites W2468904698 @default.
• W2018203142 cites W38947021 @default.
• W2018203142 cites W2154322752 @default.
• W2018203142 doi "https://doi.org/10.1016/s0016-5085(03)00694-2" @default.
• W2018203142 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/12851878" @default.
• W2018203142 hasPublicationYear "2003" @default.
• W2018203142 type Work @default.
• W2018203142 sameAs 2018203142 @default.
• W2018203142 citedByCount "9" @default.
• W2018203142 countsByYear W20182031422012 @default.
• W2018203142 countsByYear W20182031422023 @default.
• W2018203142 crossrefType "journal-article" @default.
• W2018203142 hasAuthorship W2018203142A5000033590 @default.
• W2018203142 hasAuthorship W2018203142A5010623196 @default.
• W2018203142 hasAuthorship W2018203142A5025492450 @default.
• W2018203142 hasAuthorship W2018203142A5037408048 @default.
• W2018203142 hasAuthorship W2018203142A5048500290 @default.
• W2018203142 hasAuthorship W2018203142A5051065694 @default.
• W2018203142 hasAuthorship W2018203142A5052154744 @default.
• W2018203142 hasAuthorship W2018203142A5054158772 @default.
• W2018203142 hasAuthorship W2018203142A5056582101 @default.
• W2018203142 hasAuthorship W2018203142A5058796557 @default.
• W2018203142 hasAuthorship W2018203142A5076928480 @default.
• W2018203142 hasAuthorship W2018203142A5082448644 @default.
• W2018203142 hasAuthorship W2018203142A5088345375 @default.
• W2018203142 hasAuthorship W2018203142A5091033546 @default.
• W2018203142 hasBestOaLocation W20182031421 @default.
• W2018203142 hasConcept C126322002 @default.
• W2018203142 hasConcept C134018914 @default.
• W2018203142 hasConcept C153939273 @default.
• W2018203142 hasConcept C170493617 @default.
• W2018203142 hasConcept C185592680 @default.
• W2018203142 hasConcept C2776246183 @default.
• W2018203142 hasConcept C2777148285 @default.
• W2018203142 hasConcept C2777902427 @default.
• W2018203142 hasConcept C2779591629 @default.
• W2018203142 hasConcept C2780354107 @default.

• next