Your search keyword '"Glinghammar, Björn"' showing total 4 results

1. Keratin-18 and micro RNA-122 complement alanine aminotransferase as novel safety biomarkers for drug-induced liver injury in two human cohorts.

Author

Thulin, Petra, Nordahl, Gunnar, Gry, Marcus, Yimer, Getnet, Aklillu, Eleni, Makonnen, Eyasu, Aderaye, Getachew, Lindquist, Lars, Mattsson, C. Mikael, Ekblom, Björn, Antoine, Daniel J., Park, B. Kevin, Linder, Stig, Harrill, Alison H., Watkins, Paul B., Glinghammar, Björn, and Schuppe‐Koistinen, Ina

Subjects

BIOMARKERS, LIVER injuries, ALANINE aminotransferase, MICRORNA genetics, GLUTAMATE dehydrogenase, ACETAMINOPHEN

Abstract

Background & Aims There is a demand for more sensitive, specific and predictive biomarkers for drug-induced liver injury ( DILI) than the gold standard used today, alanine aminotransferase ( ALT). The aim of this study was to qualify novel DILI biomarkers (keratin-18 markers M65/M30, micro RNA-122, glutamate dehydrogenase and alpha-foetoprotein) in human DILI. Methods Levels of the novel biomarkers were measured by enzyme-linked immunosorbent assay or real-time quantitative reverse-transcription PCR ( qRT-PCR) in two human DILI cohorts: a human volunteer study with acetaminophen and a human immunodeficiency virus (HIV)/tuberculosis (TB) study. Results In the acetaminophen study, serum M65 and micro RNA-122 levels were significantly increased at an earlier time point than ALT. Furthermore, the maximal elevation of M65 and micro RNA-122 exceeded the increase in ALT. In the HIV/ TB study, all the analysed novel biomarkers increased after 1 week of treatment. In contrast to ALT, the novel biomarkers remained stable in a human cohort with exercise-induced muscular injury. Conclusions M65 and micro RNA-122 are potential biomarkers of DILI superior to ALT with respect to sensitivity and specificity. [ABSTRACT FROM AUTHOR]

Published

2014

2. A systems biology approach to understanding elevated serum alanine transaminase levels in a clinical trial with ximelagatran.

Author

Andersson, Ulf, Lindberg, Johan, Wang, Shunghuang, Balasubramanian, Raji, Marcusson-Ståhl, Maritha, Hannula, Mira, Zeng, Chenhui, Juhasz, Peter J., Kolmert, Johan, Bäckström, Jonas, Nord, Lars, Nilsson, Kerstin, Martin, Steve, Glinghammar, Björn, Cederbrant, Karin, and Schuppe-Koistinen, Ina

Subjects

SERUM, ALANINE, CLINICAL trials, BIOMARKERS, CELL culture

Abstract

Ximelagatran was developed for the prevention and treatment of thromboembolic conditions. However, in long-term clinical trials with ximelagatran, the liver injury marker, alanine aminotransferase (ALT) increased in some patients. Analysis of plasma samples from 134 patients was carried out using proteomic and metabolomic platforms, with the aim of finding predictive biomarkers to explain the ALT elevation. Analytes that were changed after ximelagatran treatment included 3-hydroxybutyrate, pyruvic acid, CSF1R, Gc-globulin, L-glutamine, protein S and alanine, etc. Two of these analytes (pyruvic acid and CSF1R) were studied further in human cell cultures in vitro with ximelagatran. A systems biology approach applied in this study proved to be successful in generating new hypotheses for an unknown mechanism of toxicity. [ABSTRACT FROM AUTHOR]

Published

2009

3. 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

4. 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