Your search keyword '"Glinghammar, Björn"' showing total 3 results

1. A longitudinal assessment of miR-122 and GLDH as biomarkers of drug-induced liver injury in the rat.

Author

Thulin, Petra, Hornby, Robert J., Auli, Mariona, Nordahl, Gunnar, Antoine, Daniel J., Starkey Lewis, Philip, Goldring, Christopher E., Park, B. Kevin, Prats, Neus, Glinghammar, Björn, and Schuppe-Koistinen, Ina

Subjects

LIVER injuries, BIOMARKERS, AMINOTRANSFERASES, LABORATORY mice, HEPATOTOXICOLOGY

Abstract

Context:There is an ongoing search for specific and translational biomarkers of drug-induced liver injury (DILI). MicroRNA-122 (miR-122) has previously shown potential as a sensitive, specific, and translational biomarker of DILI in both rodent, and human studies. Objective:To build on previous work within the field, we examined biomarker kinetics in a rat model of acetaminophen (APAP)-induced liver injury to confirm the sensitivity, and specificity of miR-122 and glutamate dehydrogenase (GLDH). Materials and methods:qRT-PCR and a standard enzymatic assay were used for biomarker analysis. Results:Both miR-122 and GLDH were demonstrated to be more readily-detectable biomarkers of APAP-DILI than alanine aminotransferase (ALT). Peak levels for all biomarkers were detected at 2 days after APAP. At day 3, miR-122 had returned to baseline; however, other biomarkers remained elevated between 3 and 4 days. We were also able to demonstrate that, although miR-122 is present in greater quantities in exosome-free form, both exosome-bound and non-vesicle bound miR-122 are released in a similar profile throughout the course of DILI. Discussion and conclusions:Together, this study demonstrates that both GLDH and miR-122 could be used during preclinical drug-development as complementary biomarkers to ALT to increase the chance of early detection of hepatotoxicity. [ABSTRACT FROM AUTHOR]

Published

2017

2. PPARα regulates the hepatotoxic biomarker alanine aminotransferase (ALT1) gene expression in human hepatocytes

Author

Thulin, Petra, Rafter, Ingalill, Stockling, Kenneth, Tomkiewicz, Celine, Norjavaara, Ensio, Aggerbeck, Martine, Hellmold, Heike, Ehrenborg, Ewa, Andersson, Ulf, Cotgreave, Ian, and Glinghammar, Björn

Subjects

*LIVER cells, *ALANINE aminotransferase, *GENETIC regulation, *MESSENGER RNA

Abstract

Abstract: In this work, we investigated a potential mechanism behind the observation of increased aminotransferase levels in a phase I clinical trial using a lipid-lowering drug, the peroxisome proliferator-activated receptor (PPAR) α agonist, AZD4619. In healthy volunteers treated with AZD4619, serum alanine aminotransferase (ALT) and aspartate aminotransferase (AST) activities were elevated without an increase in other markers for liver injury. These increases in serum aminotransferases have previously been reported in some patients receiving another PPARα agonist, fenofibrate. In subsequent in vitro studies, we observed increased expression of ALT1 protein and mRNA in human hepatocytes after treatment with fenofibric acid. The PPAR effect on ALT1 expression was shown to act through a direct transcriptional mechanism involving at least one PPAR response element (PPRE) in the proximal ALT1 promoter, while no effect of fenofibrate and AZD4619 was observed on the ALT2 promoter. Binding of PPARs to the PPRE located at −574 bp from the transcriptional start site was confirmed on both synthetic oligonucleotides and DNA in hepatocytes. These data show that intracellular ALT expression is regulated by PPAR agonists and that this mechanism might contribute to increased ALT activity in serum. [Copyright &y& Elsevier]

Published

2008

3. Isoforms of alanine aminotransferases in human tissues and serum—Differential tissue expression using novel antibodies

Author

Lindblom, Per, Rafter, Ingalill, Copley, Clive, Andersson, Ulf, Hedberg, Jesper J., Berg, Anna-Lena, Samuelsson, Anders, Hellmold, Heike, Cotgreave, Ian, and Glinghammar, Björn

Subjects

*ALANINE, *AMINOTRANSFERASES, *TISSUES, *IMMUNOGLOBULINS, *HEPATOTOXICOLOGY

Abstract

Abstract: Serum alanine aminotransferase (ALT) is used as a clinical marker of hepatotoxicity. Two forms of ALT have been identified, ALT1 and ALT2, encoded by separate genes. The cellular and tissue distribution of the different ALT proteins has not been characterized in humans, and their relative contribution to serum is unknown. Here, we describe the development of novel isoenzyme specific ALT1 and ALT2 antibodies and the expression of the enzymes in human cells and organs. In normal human tissue, high expression of ALT1 was found in liver, skeletal muscle and kidney and low levels in heart muscle and not detectable in pancreas. High ALT2 reactivity was detected in heart and skeletal muscle, while no ALT2 expression was found in liver or kidney. Using immunohistochemistry, strong ALT1 reactivity was found in hepatocytes, renaltubular epithelial cells and in salivary gland epithelial cells, while ALT2 was expressed in adrenal gland cortex, neuronal cell bodies, cardiac myocytes, skeletal muscle fibers and endocrine pancreas. Immunoprecipitation using ALT antibodies on normal human serums showed ALT1 to be mainly responsible for basal ALT activity. Together, the results points to a differential expression of ALT1 and ALT2 in human organs and substantiate a need for investigations regarding the possible impacts on ALT measurements. [Copyright &y& Elsevier]

Published

2007