FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2022108520> ?p ?o ?g. }

• W2022108520 endingPage "333" @default.
• W2022108520 startingPage "323" @default.
• W2022108520 abstract "In vitro digestion testing is of practical importance to predict the fate of drugs administered in lipid-based delivery systems. Calcium ions are often added to digestion media to increase the extent of digestion of long-chain triglycerides (LCTs), but the effects they have on phase behaviour of the products of digestion, and consequent drug solubilization, are not well understood. This study investigates the effect of calcium and bile salt concentrations on the rate and extent of in vitro digestion of soybean oil, as well as the solubilizing capacity of the digestion products for two poorly water-soluble drugs, fenofibrate and danazol. In the presence of higher concentrations of calcium ions, the solubilization capacities of the digests were reduced for both drugs. This effect is attributed to the formation of insoluble calcium soaps, visible as precipitates during the digestions. This reduces the availability of liberated fatty acids to form mixed micelles and vesicles, thereby reducing drug solubilization. The use of high calcium concentrations does indeed force in vitro digestion of LCTs but may overestimate the extent of drug precipitation that occurs within the intestinal lumen." @default.
• W2022108520 created "2016-06-24" @default.
• W2022108520 creator A5029944399 @default.
• W2022108520 creator A5033314447 @default.
• W2022108520 creator A5037277601 @default.
• W2022108520 creator A5064072022 @default.
• W2022108520 creator A5064364780 @default.
• W2022108520 creator A5066746269 @default.
• W2022108520 date "2013-01-01" @default.
• W2022108520 modified "2023-10-18" @default.
• W2022108520 title "In vitro digestion testing of lipid-based delivery systems: Calcium ions combine with fatty acids liberated from triglyceride rich lipid solutions to form soaps and reduce the solubilization capacity of colloidal digestion products" @default.
• W2022108520 cites W1492152449 @default.
• W2022108520 cites W1513475721 @default.
• W2022108520 cites W1535579925 @default.
• W2022108520 cites W1593290141 @default.
• W2022108520 cites W1603516624 @default.
• W2022108520 cites W1751441418 @default.
• W2022108520 cites W1841280571 @default.
• W2022108520 cites W1900721369 @default.
• W2022108520 cites W1905174418 @default.
• W2022108520 cites W1967258362 @default.
• W2022108520 cites W1972553581 @default.
• W2022108520 cites W1974396612 @default.
• W2022108520 cites W1977473496 @default.
• W2022108520 cites W1979049827 @default.
• W2022108520 cites W1982850986 @default.
• W2022108520 cites W1988733774 @default.
• W2022108520 cites W1989426152 @default.
• W2022108520 cites W1990551300 @default.
• W2022108520 cites W1996669541 @default.
• W2022108520 cites W1997106286 @default.
• W2022108520 cites W2001807364 @default.
• W2022108520 cites W2003026126 @default.
• W2022108520 cites W2018053443 @default.
• W2022108520 cites W2031550786 @default.
• W2022108520 cites W2036728726 @default.
• W2022108520 cites W2039513160 @default.
• W2022108520 cites W2040127412 @default.
• W2022108520 cites W2041016731 @default.
• W2022108520 cites W2044429169 @default.
• W2022108520 cites W2048883334 @default.
• W2022108520 cites W2051046559 @default.
• W2022108520 cites W2053059620 @default.
• W2022108520 cites W2056995570 @default.
• W2022108520 cites W2058999303 @default.
• W2022108520 cites W2060751341 @default.
• W2022108520 cites W2069235788 @default.
• W2022108520 cites W2070511172 @default.
• W2022108520 cites W2071847607 @default.
• W2022108520 cites W2073996477 @default.
• W2022108520 cites W2079495578 @default.
• W2022108520 cites W2081155517 @default.
• W2022108520 cites W2082502730 @default.
• W2022108520 cites W2083034643 @default.
• W2022108520 cites W2083117601 @default.
• W2022108520 cites W2084801633 @default.
• W2022108520 cites W2085197817 @default.
• W2022108520 cites W2089926889 @default.
• W2022108520 cites W2094152940 @default.
• W2022108520 cites W2102239141 @default.
• W2022108520 cites W2117577270 @default.
• W2022108520 cites W2117725095 @default.
• W2022108520 cites W2122280404 @default.
• W2022108520 cites W2122956338 @default.
• W2022108520 cites W2123187284 @default.
• W2022108520 cites W2133061394 @default.
• W2022108520 cites W2133132084 @default.
• W2022108520 cites W2144262303 @default.
• W2022108520 cites W2158793287 @default.
• W2022108520 cites W2159300855 @default.
• W2022108520 cites W2159913680 @default.
• W2022108520 cites W2186182284 @default.
• W2022108520 cites W2206309247 @default.
• W2022108520 cites W2317799291 @default.
• W2022108520 cites W2333000505 @default.
• W2022108520 cites W2614920145 @default.
• W2022108520 cites W4253841870 @default.
• W2022108520 cites W52066678 @default.
• W2022108520 cites W63675081 @default.
• W2022108520 doi "https://doi.org/10.1016/j.ijpharm.2012.11.024" @default.
• W2022108520 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/23178598" @default.
• W2022108520 hasPublicationYear "2013" @default.
• W2022108520 type Work @default.
• W2022108520 sameAs 2022108520 @default.
• W2022108520 citedByCount "108" @default.
• W2022108520 countsByYear W20221085202013 @default.
• W2022108520 countsByYear W20221085202014 @default.
• W2022108520 countsByYear W20221085202015 @default.
• W2022108520 countsByYear W20221085202016 @default.
• W2022108520 countsByYear W20221085202017 @default.
• W2022108520 countsByYear W20221085202018 @default.
• W2022108520 countsByYear W20221085202019 @default.
• W2022108520 countsByYear W20221085202020 @default.
• W2022108520 countsByYear W20221085202021 @default.
• W2022108520 countsByYear W20221085202022 @default.
• W2022108520 countsByYear W20221085202023 @default.
• W2022108520 crossrefType "journal-article" @default.
• W2022108520 hasAuthorship W2022108520A5029944399 @default.

• next