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Recent "bile" articles

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Targetting bile-acid signalling in metabolic disease
www.nature.com
Posted by kalexflet20 to bile acids on Wed Dec 31 2008 at 15:29 UTC | info | related
 
Pharmacokinetics and metabolism of the prodrug DB289 (2,5-bis[4-(N-methoxyamidino)phenyl]furan monomaleate) in rat and monkey and its conversion to the antiprotozoal/antifungal drug DB75 (2,5-bis(4-guanylphenyl)furan dihydrochloride).
Ian Midgley et al.
Drug metabolism and disposition: the biological fate of chemicals 35 (6), 955-67 (Jun 2007)
DB289 (pafuramidine maleate; 2,5-bis[4-(N-methoxyamidino)phenyl]furan monomaleate) is a prodrug of DB75 (furamidine dihydrochloride; 2,5-bis(4-guanylphenyl)furan dihydrochloride), an aromatic dication related to pentamidine that has demonstrated good efficacy against African trypanosomiasis, Pneumocystis carinii pneumonia, and malaria, but lacks adequate oral availability. The pharmacokinetics and metabolism of 14C-DB289 have been investigated in rat and monkey after oral and intravenous administration. Oral doses were well absorbed (approximately 50-70%) and effectively converted to DB75 in both species but subject to first-pass metabolism and hepatic retention, limiting its systemic bioavailability to 10 to 20%. Clearance of DB289 approximated the liver plasma flow and its large volume of distribution was consistent with extensive tissue binding. Plasma protein binding of DB289 was 97 to 99% in four animal species and humans, but that of DB75 was noticeably less and more species- and concentration-dependent. Together, prodrug and active metabolite accounted for less than 20% of the plasma radioactivity after an oral dose, but DB75 was the major radiochemical component in key organs such as brain and liver and was largely responsible for the persistence of 14C in the body. The predominant route of excretion of radioactivity was via the feces, although biliary secretion was not particularly extensive. High-performance liquid chromatography and liquid chromatography-mass spectrometry investigations showed that the formation of DB75 from the prodrug involved the sequential loss of the two N-methoxy groups, either directly or by O-demethylation followed by reduction of the resulting oxime to the amidine. It was estimated that almost half of an oral dose of DB289 to rats and about one-third of that to monkeys was metabolized to DB75.
 
Snake bile tox (mechanism)
www.sciencedirect.com
Posted by rxwang to (mechanism) bile snake tox on Tue Sep 16 2008 at 18:31 UTC | info | related
 
Targeting bile-acid signalling for metabolic diseases
Nature Reviews Drug Discovery 7 (8), 678 (2008)
Posted by astra65 to bile on Tue Aug 12 2008 at 12:04 UTC | info | related
 
Studies of the enterohepatic circulation of morphine in the rat
C T Walsh and R R Levine
The Journal of pharmacology and experimental therapeutics 195 (2), 303-10 (Nov 1975)
 
The effect of lincomycin on the excretion of diethylstilbestrol and its uterotrophic action in rats
C T Walsh, J F Feierabend, and R R Levine
Life sciences 16 (11), 1683-8 (01 Jun 1975)
 
Adverse effects of systemic opioid analgesics
S. Schug, D. Zech, and S. Grond
DRUG SAF. 7 (3), 200-13 (1992)
 
Anatomic Variants of the Biliary Tree: MR Cholangiographic Findings and Clinical Applications
Koenraad Mortele and Pablo Ros
American Journal of Roentgenology 177 (2), 389-94 (01 Aug 2001)
Posted by f76 to bile mr MRI Anatomy on Wed Sep 05 2007 at 09:00 UTC | info | related
 
MR Imaging of Acute Biliary Disorders
Yuji Watanabe et al.
RadioGraphics 27 (2), 477-95 (01 Mar 2007)
Posted by f76 to galla bile mr MRI on Tue Sep 04 2007 at 14:01 UTC | info | related
 
Congenital cystic dilatation of the common bile duct: relationship to anomalous pancreaticobiliary ductal union
K Kimura et al.
American Journal of Roentgenology 128 (4), 571-7 (01 Apr 1977)
Posted by f76 to galla duct CBD bile abdomen on Thu Aug 02 2007 at 10:41 UTC | info | related

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