Your search keyword '"Szekeres Ferenc"' showing total 2 results

1. Digitoxin Affects Metabolism, ROS Production and Proliferation in Pancreatic Cancer Cells Differently Depending on the Cell Phenotype

Author

Lindholm, Heléne, Ejeskär, Katarina, and Szekeres, Ferenc

Subjects

Medicin och hälsovetenskap, Klinisk laboratoriemedicin, cell proliferation, Clinical Laboratory Medicine, pancreatic cancer, KRAS, PDAC, ROS, digitoxin, metabolism, Medical and Health Sciences, cardiac glycosides

Abstract

Digitoxin has repeatedly shown to have negative effects on cancer cell viability; however, the actual mechanism is still unknown. In this study, we investigated the effects of digitoxin (1-100 nM) in four pancreatic cancer cell lines, BxPC-3, CFPAC-1, Panc-1, and AsPC-1. The cell lines differ in their KRAS/BRAF mutational status and primary tumor or metastasis origin. We could detect differences in the basal rates of cell proliferation, glycolysis, and ROS production, giving the cell lines different phenotypes. Digitoxin treatment induced apoptosis in all four cell lines, but to different degrees. Cells derived from primary tumors (Panc-1 and BxPC-3) were highly proliferating with a high proportion of cells in the S/G2 phase, and were more sensitive to digitoxin treatment than the cell lines derived from metastases (CFPAC-1 and AsPC-1), with a high proportion of cells in G0/G1. In addition, the effects of digitoxin on the rate of glycolysis, ROS production, and proliferation were dependent on the basal metabolism and origin of the cells. The KRAS downstream signaling pathways were not altered by digitoxin treatment, thus the effects exerted by digitoxin were probably disconnected from these signaling pathways. We conclude that digitoxin is a promising treatment in highly proliferating pancreatic tumors. CC BY 4.0Correspondence: ferenc.szekeres@his.seFunding: This research was funded by Assar Gabrielsson Foundation, grant FB19-80.

Published

2022

2. TWIST1 and TWIST2 regulate glycogen storage and inflammatory genes in skeletal muscle.

Author

Mudry, Jonathan M., Massart, Julie, Szekeres, Ferenc L. M., and Krook, Anna

Subjects

SKELETAL muscle, GLYCOGEN storage disease, GENETIC regulation, ADIPOSE tissue tumors, GENETIC overexpression

Abstract

TWIST proteins are important for development of embryonic skeletal muscle and play a role in the metabolism of tumor and white adipose tissue. The impact of TWIST on metabolism in skeletal muscle is incompletely studied. Our aim was to assess the impact of TWIST1 and TWIST2 overexpression on glucose and lipid metabolism. In intact mouse muscle, overexpression of Twist reduced total glycogen content without altering glucose uptake. Expression of TWIST or TWIST2 reduced Pdk4 mRNA, while increasing mRNA levels of 116, Tnfα, and Il1β. Phosphorylation of AKT was increased and protein abundance of acetyl CoA carboxylase (ACC) was decreased in skeletal muscle overexpressing TWIST1 or TWIST2. Glycogen synthesis and fatty acid oxidation remained stable in C2C12 cells overexpressing TWIST1 or TWIST2. Finally, skeletal muscle mRNA levels remain unaltered in ob/ob mice, type 2 diabetic patients, or in healthy subjects before and after 3 months of exercise training. Collectively, our results indicate that TWIST1 and TWIST2 are expressed in skeletal muscle. Overexpression of these proteins impacts proteins in metabolic pathways and mRNA level of cytokines. However, skeletal muscle levels of TWIST transcripts are unaltered in metabolic diseases. [ABSTRACT FROM AUTHOR]

Published

2015