FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W3149939461> ?p ?o ?g. }

• W3149939461 abstract "Until recently knowledge of oxalate metabolism has been hampered by problems in the measurement of oxalate in urine, plasma and other body fluids. The studies described in this thesis were directed towards the development of simple sensitive assays for oxalate, which could then be used to investigate oxalate metabolism in normal subjects and idiopathic calcium oxalate stone formers. An evaluation was performed of several possible methods. The definitive method developed was a solvent generated ion exchange chromatographic system with electrochemical detection. Acidified urine was pretreated by dilution with neutral phosphate buffer and passage through a C18 cartridge. Stabilised plasma was diluted with neutral acetate buffer and oxalate extracted using a strong anion exchange cartridge. Plasma samples were stabilised with the reducing agent dithiothreitol. There was no significant protein binding of oxalate at physiological pH. Reference ranges were established for urine and plasma oxalate, and also for renal clearance and fractional excretion. Fasting lowered plasma and urine oxalate ranges and renal handling was modified by diet. Studies on normal subjects revealed no diurnal variation in urine oxalate but plasma oxalate decreased overnight. Oxalate loading in normal subjects demonstrated renal adaptation to the load, with net renal reabsorption of oxalate becoming net secretion. These studies suggest that the main site of oxalate absorption is the small intestine. It was found that increasing the load beyond a critical level did not increase the absorption, indicating a limited capacity. Oxalate loading did not effect ketogenesis in normal subjects and loading with ascorbic acid (1g), an oxalate precursor, did not alter urine or plasma oxalate levels. Idiopathic calcium oxalate stone formers showed a 22. 8% incidence of hyperoxaluria, although the frequency of hyperoxaluria within individuals varied. Hyperoxaluria was associated with hyperuricosuria, hypercalciuria and high urinary creatinine output in the fed state, but not on fasting. Hyperoxalurics had a net tubular secretion of oxalate in the fasting state, suggesting a renally mediated loss, delayed gut absorption or increased endogenous production of oxalate." @default.
• W3149939461 created "2021-04-13" @default.
• W3149939461 creator A5017115922 @default.
• W3149939461 date "1991-01-01" @default.
• W3149939461 modified "2023-09-27" @default.
• W3149939461 title "Oxalate analysis and its applications." @default.
• W3149939461 hasPublicationYear "1991" @default.
• W3149939461 type Work @default.
• W3149939461 sameAs 3149939461 @default.
• W3149939461 citedByCount "0" @default.
• W3149939461 crossrefType "dissertation" @default.
• W3149939461 hasAuthorship W3149939461A5017115922 @default.
• W3149939461 hasConcept C179104552 @default.
• W3149939461 hasConcept C185592680 @default.
• W3149939461 hasConcept C2776179656 @default.
• W3149939461 hasConcept C2776351790 @default.
• W3149939461 hasConcept C2780026642 @default.
• W3149939461 hasConcept C2781346138 @default.
• W3149939461 hasConcept C2986274086 @default.
• W3149939461 hasConcept C31903555 @default.
• W3149939461 hasConcept C43617362 @default.
• W3149939461 hasConcept C55493867 @default.
• W3149939461 hasConceptScore W3149939461C179104552 @default.
• W3149939461 hasConceptScore W3149939461C185592680 @default.
• W3149939461 hasConceptScore W3149939461C2776179656 @default.
• W3149939461 hasConceptScore W3149939461C2776351790 @default.
• W3149939461 hasConceptScore W3149939461C2780026642 @default.
• W3149939461 hasConceptScore W3149939461C2781346138 @default.
• W3149939461 hasConceptScore W3149939461C2986274086 @default.
• W3149939461 hasConceptScore W3149939461C31903555 @default.
• W3149939461 hasConceptScore W3149939461C43617362 @default.
• W3149939461 hasConceptScore W3149939461C55493867 @default.
• W3149939461 hasLocation W31499394611 @default.
• W3149939461 hasOpenAccess W3149939461 @default.
• W3149939461 hasPrimaryLocation W31499394611 @default.
• W3149939461 hasRelatedWork W1001282899 @default.
• W3149939461 hasRelatedWork W107406080 @default.
• W3149939461 hasRelatedWork W1692169222 @default.
• W3149939461 hasRelatedWork W194123058 @default.
• W3149939461 hasRelatedWork W2005290060 @default.
• W3149939461 hasRelatedWork W2028294619 @default.
• W3149939461 hasRelatedWork W2089115492 @default.
• W3149939461 hasRelatedWork W2096157690 @default.
• W3149939461 hasRelatedWork W2148808200 @default.
• W3149939461 hasRelatedWork W2309283936 @default.
• W3149939461 hasRelatedWork W2414577119 @default.
• W3149939461 hasRelatedWork W2467601753 @default.
• W3149939461 hasRelatedWork W247371833 @default.
• W3149939461 hasRelatedWork W2487418693 @default.
• W3149939461 hasRelatedWork W2507273309 @default.
• W3149939461 hasRelatedWork W251288464 @default.
• W3149939461 hasRelatedWork W2794656273 @default.
• W3149939461 hasRelatedWork W749185240 @default.
• W3149939461 hasRelatedWork W89287402 @default.
• W3149939461 hasRelatedWork W2401262006 @default.
• W3149939461 isParatext "false" @default.
• W3149939461 isRetracted "false" @default.
• W3149939461 magId "3149939461" @default.
• W3149939461 workType "dissertation" @default.