Predictive value of random sample urine bile acids corrected by creatinine in liver disease

Simko, Vlado; Michael, Shoukry; Kelley, Robin D. G.

doi:10.1002/hep.1840070123

Cited by 24 publications

(34 citation statements)

References 21 publications

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“…First, although urinary BA analysis is not performed in the laboratories of most hospitals, it should be included in routine investigational assays of chronic cholestatic patients, as expanded lists of phenotypic and metabolic defects associated with IEBAM have been recently reported (30). In clinical practice, urine sample collection is easy to perform, the data are not affected by fasting conditions after correction by Cre, and analyses have low variability and high stability compared with analyses of serum BAs levels (31,32).…”

Section: Discussionmentioning

confidence: 99%

Prognostic roles of tetrahydroxy bile acids in infantile intrahepatic cholestasis

Lee

Kimura

et al. 2017

Journal of Lipid Research

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Section: Discussionmentioning

confidence: 99%

Prognostic roles of tetrahydroxy bile acids in infantile intrahepatic cholestasis

Lee

Kimura

et al. 2017

Journal of Lipid Research

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“…11 Similarly, specific markers of liver injury have been proposed, for example, urinary levels of bile acids have been proposed as non-invasive markers of minor liver dysfunction which are as sensitive as serum measurements. 32 Elevations in the levels of urinary taurine have also been associated with liver dysfunction. 27,33 However, many endogenous metabolites, such as taurine, fluctuate in concentration as a result of normal physiological variation.…”

Section: Nmr Based Metabonomicsmentioning

confidence: 99%

NMR-based metabonomic approaches for evaluating physiological influences on biofluid composition

et al. 2004

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Strategies such as genomics, proteomics and metabonomics are being applied with increasing frequency in the pharmaceutical industry. For each of these approaches, toxicological response can be measured by terms of deviation from control or baseline status. However, in order to accurately define drug-induced response, it is necessary to characterize the normal degree of physiological variation in the absence of stimuli. Here, 1 H NMR spectroscopic-based analyses of the metabolic composition of urine in experimental animals under various normal physiological conditions are reviewed. In particular, the effects of inter-animal and diurnal variation, gender, age, diet, species, strain, hormonal status and stress on the biochemical composition of urine are explored. Pattern recognition methods facilitate the comparison of urine NMR spectra over a given time-course, enabling the establishment of changes in profile and highlighting the dynamic metabolic status of an organism. Thus metabonomic approaches based on information-rich spectroscopic data sets can be used to evaluate normal physiological variation and for investigation of drug safety issues.

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“…Urine bile acids (UBA) have been detected in patients with hepatic disease since the 1950s (Rudman and Kendall, 1957; Makino et al et al., 1976;Almé et al, 1977;Simko et al, 1987;Batta et al, 1989; Shoda et al acids has been carried out mainly by gas or liquid chromatography -mass spectrometry (GC-MS, LC-MS) in recent studies. GC-MS and LC-MS can identify various structurally different bile acids precisely, and alteration of the composition of UBA can be analyzed.…”

Section: Original Articlementioning

confidence: 99%

“…Normalized UBA values were expressed in micromoles per gram of creat--atinine, because this method was generally used in order to normalize the amount of urinary compounds, and several studies revealed that this normalization was suitable for UBA analysis in human, cats, and dogs (Simko et al, 1987;Trainor et al, 2003;Balkman et al, 2003).…”

Section: Original Articlementioning

confidence: 99%

“…The blood concentration -tions, but is increased in the case of a disorder in the liver or biliary tract (Dawson, 2002). Therefore, the serum bile acid level is a marker of liver disease, although it is not widely used as a routine screening test.Urine bile acids (UBA) have been detected in patients with hepatic disease since the 1950s (Rudman and Kendall, 1957; Makino et al et al., 1976;Almé et al, 1977;Simko et al, 1987;Batta et al, 1989; Shoda et al acids has been carried out mainly by gas or liquid chromatography -mass spectrometry (GC-MS, LC-MS) in recent studies. GC-MS and LC-MS can identify various structurally different bile acids precisely, and alteration of the composition of UBA can be analyzed.…”

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confidence: 99%

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Efficacy of urine bile acid as a non-invasive indicator of liver damage in rats

et al. 2009

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-Estimation of liver damage is important in the pathophysiological and toxicological bile acids (UBA) in a rat model of liver disease. Thioacetamide (TAA)-treated rats were used in this study. Single intraperitoneal administration of high-dose TAA induces severe damage to the liver, and thus is used as a model of acute hepatitis. Continuous administration of low-dose TAA yields mild damand chronic administration of TAA was associated with a dose-dependent elevation of UBA. The elevation of UBA content correlated with the alteration of blood biochemical indicators, and UBA screening -with abnormal serum alkaline phosphatase (ALP) activity due to chronic liver damage, which was condemonstrated that measurement of UBA is a simple, non-invasive and effective method for the screening of cholestasis in TAA-treated rats. We suggest that UBA analysis may have potent applicability for monitoring the progress of liver damage in animal models of chronic liver disease, such as cirrhosis and hepatic encephalopathy.Bile acid, Urine, Liver, Cholestasis, Cirrhosis, ThioacetamideCorrespondence: Hiroshi Kawai (E-mail: hkawai@jiu.ac.jp) Original ArticleThe Journal of Toxicological Sciences (J. Toxicol. Sci.) Vol.34, No.1, 27-38, 2009 Vol. 34 No. 1 27 the systemic circulation is small. The blood concentration -tions, but is increased in the case of a disorder in the liver or biliary tract (Dawson, 2002). Therefore, the serum bile acid level is a marker of liver disease, although it is not widely used as a routine screening test.Urine bile acids (UBA) have been detected in patients with hepatic disease since the 1950s (Rudman and Kendall, 1957; Makino et al et al., 1976;Almé et al., 1977;Simko et al., 1987;Batta et al., 1989; Shoda et al acids has been carried out mainly by gas or liquid chromatography -mass spectrometry (GC-MS, LC-MS) in recent studies. GC-MS and LC-MS can identify various structurally different bile acids precisely, and alteration of the composition of UBA can be analyzed. These methods, however, require complicated sample preparation, a long period of time, and a well-disciplined technician. A more simple and rapid method is needed for routine screening or analysis of a large number of samples. Recently, the direct enzymatic assay of urine sulfated bile acids (USBA) content was developed as a diagnostic tool (Matsui et al., 1996), and several reports revealed the clinical importance of USBA analysis (Obatake et al., 2002; Shinohara et al., 2005; Huang et al., 2007). Since a large portion of bile acids are sulfated in human urine (Palmer, 1967;Stiehl, 1974), USBA rather than non-sulfated UBA is useful in clinical application.UBA has also been analyzed in various animal species, such as hamsters (Galeazzi and Javitt, 1977), chimpanzees (Schweng et al., 1978), rabbits (Nakao et al., 1980), monkeys (Suzuki et al., 1985), and rats (Palmer, 1971; Takita et al., 1988;Lee et al., 2001). However, these studies focused on the alteration of metabolic ability of the liver and the pathogenic mechanisms of liver disease...

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Predictive value of random sample urine bile acids corrected by creatinine in liver disease

Cited by 24 publications

References 21 publications

Prognostic roles of tetrahydroxy bile acids in infantile intrahepatic cholestasis

Prognostic roles of tetrahydroxy bile acids in infantile intrahepatic cholestasis

NMR-based metabonomic approaches for evaluating physiological influences on biofluid composition

Efficacy of urine bile acid as a non-invasive indicator of liver damage in rats

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