FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1157291229> ?p ?o ?g. }

• W1157291229 abstract "Background: Vascular access dysfunction associated with arteriovenous grafts and fistulas contributes significantly to the morbidity and mortality of end-stage renal disease (ESRD) patients receiving hemodialysis. The mechanism involved in the development of peri-anastomotic intimal hyperplasia, a major cause of the arteriovenous access dysfunction, is poorly elucidated. We hypothesized that the uremic condition associated with ESRD promotes a pathophysiological vascular smooth muscle cell (VSMC) phenotype that contributes to accelerated development of intimal hyperplasia in blood vessels, both de novo and following the arteriovenous anastomosis. Methods and Results: We examined the effect of culturing human VSMC with human uremic serum on its phenotype. We utilized quantitative real-time PCR to measure the expression of the VSMC-specific contractile marker genes, and found that these genes were reduced 50-80% in VSMC exposed to serum from hemodialysis patients as compared to serum from patients with normal renal function. Chromatin immunoprecipitation assays demonstrated that there were also significant changes in epigenetic markers associated with contractile gene promoters in VSMC cultured in uremic conditions. Moreover, there was a 60% increase in proliferation rate in cells exposed to uremic conditions, with no change in the levels of apoptosis as compared to cells exposed to non-uremic conditions. Interestingly, uremic serum from ESRD patients inhibited PDGF-induced migration of VSMC. We also examined the histopathology of veins from patients with normal kidney function and chronic kidney disease (CKD). Indeed, we found significant de novo venous intimal hyperplasia exists in CKD and ESRD patients prior to any surgical manipulation as compared to veins from patients with normal kidney function. Conclusion: CKD alters VSMC phenotype in vitro and contributes to intimal hyperplasia formation in vivo resulting in the pathogenesis of vascular access dysfunction in ESRD patients." @default.
• W1157291229 created "2016-06-24" @default.
• W1157291229 creator A5000169183 @default.
• W1157291229 creator A5004366207 @default.
• W1157291229 creator A5006264565 @default.
• W1157291229 creator A5015377299 @default.
• W1157291229 creator A5024467260 @default.
• W1157291229 creator A5065816864 @default.
• W1157291229 creator A5085121775 @default.
• W1157291229 date "2014-05-01" @default.
• W1157291229 modified "2023-10-16" @default.
• W1157291229 title "Abstract 347: Chronic Kidney Disease Modulates Vascular Smooth Muscle Cell Phenotype and Increases de Novo Venous Intimal Hyperplasia" @default.
• W1157291229 doi "https://doi.org/10.1161/atvb.34.suppl_1.347" @default.
• W1157291229 hasPublicationYear "2014" @default.
• W1157291229 type Work @default.
• W1157291229 sameAs 1157291229 @default.
• W1157291229 citedByCount "0" @default.
• W1157291229 crossrefType "journal-article" @default.
• W1157291229 hasAuthorship W1157291229A5000169183 @default.
• W1157291229 hasAuthorship W1157291229A5004366207 @default.
• W1157291229 hasAuthorship W1157291229A5006264565 @default.
• W1157291229 hasAuthorship W1157291229A5015377299 @default.
• W1157291229 hasAuthorship W1157291229A5024467260 @default.
• W1157291229 hasAuthorship W1157291229A5065816864 @default.
• W1157291229 hasAuthorship W1157291229A5085121775 @default.
• W1157291229 hasConcept C126322002 @default.
• W1157291229 hasConcept C134018914 @default.
• W1157291229 hasConcept C142724271 @default.
• W1157291229 hasConcept C2776635150 @default.
• W1157291229 hasConcept C2778063415 @default.
• W1157291229 hasConcept C2778653478 @default.
• W1157291229 hasConcept C2779395532 @default.
• W1157291229 hasConcept C2779751240 @default.
• W1157291229 hasConcept C2780091579 @default.
• W1157291229 hasConcept C2992686903 @default.
• W1157291229 hasConcept C3019040382 @default.
• W1157291229 hasConcept C71924100 @default.
• W1157291229 hasConceptScore W1157291229C126322002 @default.
• W1157291229 hasConceptScore W1157291229C134018914 @default.
• W1157291229 hasConceptScore W1157291229C142724271 @default.
• W1157291229 hasConceptScore W1157291229C2776635150 @default.
• W1157291229 hasConceptScore W1157291229C2778063415 @default.
• W1157291229 hasConceptScore W1157291229C2778653478 @default.
• W1157291229 hasConceptScore W1157291229C2779395532 @default.
• W1157291229 hasConceptScore W1157291229C2779751240 @default.
• W1157291229 hasConceptScore W1157291229C2780091579 @default.
• W1157291229 hasConceptScore W1157291229C2992686903 @default.
• W1157291229 hasConceptScore W1157291229C3019040382 @default.
• W1157291229 hasConceptScore W1157291229C71924100 @default.
• W1157291229 hasIssue "suppl_1" @default.
• W1157291229 hasLocation W11572912291 @default.
• W1157291229 hasOpenAccess W1157291229 @default.
• W1157291229 hasPrimaryLocation W11572912291 @default.
• W1157291229 hasRelatedWork W1157291229 @default.
• W1157291229 hasRelatedWork W1972216846 @default.
• W1157291229 hasRelatedWork W2003814064 @default.
• W1157291229 hasRelatedWork W2024344073 @default.
• W1157291229 hasRelatedWork W2055444814 @default.
• W1157291229 hasRelatedWork W2072979799 @default.
• W1157291229 hasRelatedWork W2073034255 @default.
• W1157291229 hasRelatedWork W2075043838 @default.
• W1157291229 hasRelatedWork W2119785961 @default.
• W1157291229 hasRelatedWork W4293585094 @default.
• W1157291229 hasVolume "34" @default.
• W1157291229 isParatext "false" @default.
• W1157291229 isRetracted "false" @default.
• W1157291229 magId "1157291229" @default.
• W1157291229 workType "article" @default.