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Thomas Durcan: I choose The Neuro

Thomas Durcan came to The Neuro to be part of its new generation and its new vision. 鈥淚t鈥檚 an exciting time to be here,鈥 he says. 鈥淣ew researchers working with older researchers 鈥 it鈥檚 very inspiring." His lab is making stem cells that can turn be turned into neurons.

Thomas M. Durcan is an assistant professor in the department of Neurology and Neurosurgery at 91社区 and is a member of the Centre for Neurodegenerative disease group at the MNI. Durcan received his Bachelor of Science from University College Dublin, Ireland, before moving to the USA where he obtained his PhD in Cell and Molecular Biology from the University of Notre Dame in 2007. For his postdoctoral research, Durcan joined the Parkinson鈥檚 research group of Dr Edward Fon, were he focused on the function of deubiquitinating enzymes in Parkinson鈥檚 disease and other neurodegenerative disorders.

His current research program is focused on the use of induced pluripotent stem cells (iPSCs) and mouse models to understand how specific pathways are affected in Parkinson鈥檚 disease and other neurodegenerative disorders. In addition to his academic appointment, Durcan manages the new Brain Canada iPSC-CRISPR translational platform at the MNI, focused on providing iPSC-derived neurons for use in different academic and translational projects. During this time, he has published in many prestigious scientific journals including Journal of Cell Biology, EMBO Journal, and Human Molecular Genetics. He has previously received research support from the Parkinson鈥檚 Society of Canada, Parkinson鈥檚 Disease Foundation and National Ataxia Foundation. He is currently funded through a research grant from the Michael J Fox Foundation. 听

Selected Publications

Roberts, R.F., Tang, M.Y., Fon E.A. and Durcan T.M. (2016) Defending the mitochondria: The pathways of mitophagy and mitochondrial-derived vesicles. International Journal of Biochemistry and Cell Biology. S1357-2725(16)30194-7

Aguileta M.A., Korac J., Durcan T.M., Trempe J.F., Haber M., Gehring K., Elsasser S., Waidmann O., Fon E.A., Husnjak K. (2015) The E3 ubiquitin ligase parkin is recruited to the 26 S proteasome via the proteasomal ubiquitin receptor Rpn13. Journal of Biological Chemistry. 290(12): 7492-505.

Durcan T.M. and Fon E.A. (2015) The three 'P's of mitophagy: PARKIN, PINK1, and post-translational modifications. Genes and Development. 29(10):989-99

Durcan T.M. and Fon E.A. (2015) USP8 and PARK2/parkin-mediated mitophagy. Autophagy. 11(2): 428-9.

Durcan T.M., Tang M.Y., P茅russe J.R., Dashti E.A., Aguileta M.A., McLelland G.L., Gros P., Shaler T.A., Faubert D., Coulombe B., Fon E.A. (2014) USP8 regulates mitophagy by removing K6-linked ubiquitin conjugates from parkin. EMBO J. 33(21): 2473-91.

Montie, H.L and Durcan, T.M. (2013) The cell and molecular biology of neurodegenerative diseases: an overview. Frontiers in Neurology 4:194. doi: 10.3389/fneur.2013.00194. eCollection 2013

Durcan, T.M. and Fon, E.A. (2013) Ataxin-3 and its E3 partners: Implications for Machado-Joseph disease, Frontiers in Neurology 4:46. doi: 10.3389/fneur.2013.00046. eCollection 2013

Durcan, T.M., Kontogiannea, M., Bedard, N., Wing, S.S. and Fon, E.A. (2012) Ataxin-3 deubiquitination is coupled to parkin ubiquitination via the E2 ubiquitin-conjugating enzyme. Journal of Biological Chemistry. 287(1): 531-41.

Durcan, T.M, Kontogiannea, M., Thorarinsdottir, T.E., Fallon, L., Fantaneanu, T.A., Williams, A.J., Paulson, H.L., Fon E.A. (2011) The Machado-Joseph disease-associated mutant form of听ataxin-3 regulates parkin ubiquitination and stability. Human Molecular Genetics. 20(1):141-54.

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The Neuro (Montreal Neurological Institute-Hospital)听is a bilingual academic healthcare institution. We are a听91社区 research and teaching institute; delivering high-quality patient care, as part of the Neuroscience Mission of the 91社区 Health Centre.听We are听proud to be a Killam Institution, supported by the Killam Trusts.

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