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19 results on '"Robinson, Claire M."'

4. The Q61H mutation decouples KRAS from upstream regulation and renders cancer cells resistant to SHP2 inhibitors

Author

Gebregiworgis, Teklab, Kano, Yoshihito, St-Germain, Jonathan, Radulovich, Nikolina, Udaskin, Molly L., Mentes, Ahmet, Huang, Richard, Poon, Betty P. K., He, Wenguang, Valencia-Sama, Ivette, Robinson, Claire M., Huestis, Melissa, Miao, Jinmin, Yeh, Jen Jen, Zhang, Zhong-Yin, Irwin, Meredith S., Lee, Jeffrey E., Tsao, Ming-Sound, Raught, Brian, Marshall, Christopher B., Ohh, Michael, and Ikura, Mitsuhiko

Published
2021
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11. Inhibition of IRE1α RNase activity sensitizes patient‐derived acute myeloid leukaemia cells to proteasome inhibitors

Author

Creedican, Stuart, primary, Robinson, Claire M., additional, Mnich, Katarzyna, additional, Islam, Md Nahidul, additional, Szegezdi, Eva, additional, Clifford, Ruth, additional, Krawczyk, Janusz, additional, Patterson, John B., additional, FitzGerald, Stephen P., additional, Summers, Mark, additional, Richardson, Ciaran, additional, Martin, Kenneth, additional, Gorman, Adrienne M., additional, and Samali, Afshin, additional

Published
2022
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15. Hypoxia-induced DNA hypermethylation in human pulmonary fibroblasts is associated with Thy-1 promoter methylation and the development of a pro-fibrotic phenotype

Author

Robinson Claire M, Neary Roisin, Levendale Ashleigh, Watson Chris J, and Baugh John A

Subjects
Hypoxia, Hypermethylation, Thy-1, Lung fibrosis, Myofibroblast, Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Pulmonary fibrosis is a debilitating and lethal disease with no effective treatment options. Understanding the pathological processes at play will direct the application of novel therapeutic avenues. Hypoxia has been implicated in the pathogenesis of pulmonary fibrosis yet the precise mechanism by which it contributes to disease progression remains to be fully elucidated. It has been shown that chronic hypoxia can alter DNA methylation patterns in tumour-derived cell lines. This epigenetic alteration can induce changes in cellular phenotype with promoter methylation being associated with gene silencing. Of particular relevance to idiopathic pulmonary fibrosis (IPF) is the observation that Thy-1 promoter methylation is associated with a myofibroblast phenotype where loss of Thy-1 occurs alongside increased alpha smooth muscle actin (α-SMA) expression. The initial aim of this study was to determine whether hypoxia regulates DNA methylation in normal human lung fibroblasts (CCD19Lu). As it has been reported that hypoxia suppresses Thy-1 expression during lung development we also studied the effect of hypoxia on Thy-1 promoter methylation and gene expression. Methods CCD19Lu were grown for up to 8 days in hypoxia and assessed for global changes in DNA methylation using flow cytometry. Real-time PCR was used to quantify expression of Thy-1, α-SMA, collagen I and III. Genomic DNA was bisulphite treated and methylation specific PCR (MSPCR) was used to examine the methylation status of the Thy-1 promoter. Results Significant global hypermethylation was detected in hypoxic fibroblasts relative to normoxic controls and was accompanied by increased expression of myofibroblast markers. Thy-1 mRNA expression was suppressed in hypoxic cells, which was restored with the demethylating agent 5-aza-2′-deoxycytidine. MSPCR revealed that Thy-1 became methylated following fibroblast exposure to 1% O2. Conclusion These data suggest that global and gene-specific changes in DNA methylation may play an important role in fibroblast function in hypoxia.

Published
2012
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17. Consequences of VHL Loss on Global DNA Methylome

Author

Robinson, Claire M., primary, Lefebvre, Francois, additional, Poon, Betty P., additional, Bousard, Aurelie, additional, Fan, Xiaojun, additional, Lathrop, Mark, additional, Tost, Jorg, additional, Kim, William Y., additional, Riazalhosseini, Yasser, additional, and Ohh, Michael, additional

Published
2018
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18. HIF-2α-pVHL complex reveals broad genotype- phenotype correlations in HIF-2α-driven disease.

Author

Tarad, Daniel, Robinson, Claire M., Lee, Jeffrey E., and Oh, Michael

Abstract

It is definitively established that mutations in transcription factor HIF-2α are causative of both neuroendocrine tumors (class 1 disease) and polycythemia (class 2 disease). However, the molecular mechanism that underlies this emergent genotype-phenotype relationship has remained unclear. Here, we report the structure of HIF-2α peptide bound to pVHL-elongin B- elongin C (VBC) heterotrimeric complex, which shows topographical demarcation of class 1 and 2 mutations affecting residues predicted, and demonstrated via biophysical analyses, to differentially impact HIF-2α-pVHL interaction interface stability. Concordantly, biochemical experiments showed that class 1 mutations disrupt pVHL affinity to HIF-2α more adversely than class 2 mutations directly or indirectly via impeding PHD2-mediated hydroxylation. These findings suggest that neuroendocrine tumor pathogenesis requires a higher HIF-2α dose than polycythemia, which requires only a mild increase in HIF-2α activity. These biophysical data reveal a structural basis that underlies, and can be used to predict de novo, broad genotype-phenotype correlations in HIF-2α-driven disease. [ABSTRACT FROM AUTHOR]

Published
2018
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