Your search keyword '"Anna Skwarska"' showing total 2 results

1. Pharmacological Inhibition of ATR Can Block Autophagy through an ATR-Independent Mechanism

Author

Elizabeth Bowler, Anna Skwarska, Joseph D. Wilson, Shaliny Ramachandran, Hannah Bolland, Alistair Easton, Christian Ostheimer, Ming-Shih Hwang, Katarzyna B. Leszczynska, Stuart J. Conway, and Ester M. Hammond

Subjects

Biological Sciences, Biochemistry, Biochemical Mechanism, Cancer, Science

Abstract

Summary: Inhibition of the ATR kinase has emerged as a therapeutically attractive means to target cancer since the development of potent inhibitors, which are now in clinical testing. We investigated a potential link between ATR inhibition and the autophagy process in esophageal cancer cells using four ATR inhibitors including two in clinical testing. The response to pharmacological ATR inhibitors was compared with genetic systems to investigate the ATR dependence of the effects observed. The ATR inhibitor, VX-970, was found to lead to an accumulation of p62 and LC3-II indicative of a blocked autophagy. This increase in p62 occurred post-transcriptionally and in all the cell lines tested. However, our data indicate that the accumulation of p62 occurred in an ATR-independent manner and was instead an off-target response to the ATR inhibitor. This study has important implications for the clinical response to pharmacological ATR inhibition, which in some cases includes the blockage of autophagy.

Published

2020

2. Pharmacological Inhibition of ATR Can Block Autophagy through an ATR-Independent Mechanism

Author

Joseph D. Wilson, Shaliny Ramachandran, Christian Ostheimer, Ester M. Hammond, Katarzyna B. Leszczynska, Ming-Shih Hwang, Hannah Bolland, Alistair Easton, Stuart J. Conway, Anna Skwarska, and Elizabeth Bowler

Subjects

0301 basic medicine, 02 engineering and technology, Pharmacology, Biochemistry, Article, 03 medical and health sciences, stomatognathic system, medicine, lcsh:Science, Biological sciences, Cancer, Multidisciplinary, Kinase, Chemistry, Mechanism (biology), Biochemical Mechanism, Autophagy, Genetic systems, Biological Sciences, 021001 nanoscience & nanotechnology, medicine.disease, 030104 developmental biology, Cell culture, lcsh:Q, biological phenomena, cell phenomena, and immunity, 0210 nano-technology, Biochemical mechanism

Abstract

Summary Inhibition of the ATR kinase has emerged as a therapeutically attractive means to target cancer since the development of potent inhibitors, which are now in clinical testing. We investigated a potential link between ATR inhibition and the autophagy process in esophageal cancer cells using four ATR inhibitors including two in clinical testing. The response to pharmacological ATR inhibitors was compared with genetic systems to investigate the ATR dependence of the effects observed. The ATR inhibitor, VX-970, was found to lead to an accumulation of p62 and LC3-II indicative of a blocked autophagy. This increase in p62 occurred post-transcriptionally and in all the cell lines tested. However, our data indicate that the accumulation of p62 occurred in an ATR-independent manner and was instead an off-target response to the ATR inhibitor. This study has important implications for the clinical response to pharmacological ATR inhibition, which in some cases includes the blockage of autophagy., Graphical Abstract, Highlights • Inhibition of ATR using VX-970 leads to an accumulation of p62 • VX-970-mediated accumulation of p62 occurs independently of ATR • VX-970-mediated accumulation of p62 is consistent with blocked autophagy, Biological Sciences; Biochemistry; Biochemical Mechanism; Cancer

Published

2020