Ben G. Davis
Ben Davis | |
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Ben Davis in 2015, portrait from the Royal Society | |
Born |
Benjamin Guy Davis 8 August 1970[1][2][3] |
Fields | |
Institutions | |
Alma mater | University of Oxford (BA, DPhil) |
Doctoral advisor | George Fleet[6] |
Other academic advisors | J. Bryan Jones[7] |
Doctoral students | |
Notable awards | |
Website users |
Benjamin Guy Davis FRS[20] (born 8 August 1970) is a Professor of Chemistry in the Department of Chemistry at the University of Oxford.[22][23][24][25][26]
Education
Davis was educated at the University of Oxford where he was awarded Bachelor of Arts and Doctor of Philosophy degrees in chemistry.[6]
Research
Davis' group's research centres on the chemical understanding and exploitation of biomolecular function (Synthetic Biology, Chemical Biology and Chemical Medicine), with an emphasis on carbohydrates and proteins. In particular, the group's interests encompass synthesis and methodology; target biomolecule synthesis; inhibitor/probe/substrate design; biocatalysis; enzyme & biomolecule mechanism; biosynthetic pathway determination; protein engineering; drug delivery; molecular biology; structural biology; cell biology; glycobiology; molecular imaging and in vivo biology.[21]
Awards and honours
Davis was elected a Fellow of the Royal Society (FRS) in 2015.[21] His certificate of election reads:
“ | Professor Davis is noted for his chemical interrogation and manipulation of biological systems, particularly those that hinge on carbohydrates and proteins. He has developed selective and benign bond forming strategies that have been applied to biology, allowing the construction of synthetic biomolecules and bioconjugates; the creation of synthetic cells and viruses; and in vivo chemistry. These have enabled associated mechanistic details of protein and sugar biology to be elucidated and exploited for biotechnological applications.[20] | ” |
References
- ↑ DAVIS, Prof. Benjamin Guy. Who's Who. 2016 (online Oxford University Press ed.). A & C Black, an imprint of Bloomsbury Publishing plc. (subscription required)
- ↑ Anon (2009). "Benjamin G. Davis". Angewandte Chemie. 48 (22): 3900. doi:10.1002/anie.200901068.
- ↑ Davis, B. (2010). "Future Visions of Chemistry: Ben Davis". ChemViews. doi:10.1002/chemv.201000012.
- ↑ Davis, B. G. (2002). "Synthesis of glycoproteins". Chemical Reviews. 102 (2): 579–602. doi:10.1021/cr0004310. PMID 11841255.
- ↑ Gamblin, David P.; Scanlan, Eoin M.; Davis, Benjamin G. (2009). "Glycoprotein Synthesis: An Update". Chemical Reviews. 109 (1): 131–163. doi:10.1021/cr078291i. ISSN 0009-2665.
- 1 2 3 "The Davis Group". University of Oxford. Archived from the original on 15 June 2013.
- ↑ Ambrosi, M; Cameron, N. R.; Davis, B. G. (2005). "Lectins: Tools for the molecular understanding of the glycocode". Organic & Biomolecular Chemistry. 3 (9): 1593–608. doi:10.1039/b414350g. PMID 15858635.
- ↑ Bhushan, Bhaskar (2014). Unnatural amino acids as metal-mediated probes of biological function (DPhil thesis). University of Oxford.
- ↑ Lercher, Lukas A. (2014). Chemical tools for the study of epigenetic mechanisms (DPhil thesis). University of Oxford. OCLC 897880623.
- ↑ Lercher, L; McGouran, J. F.; Kessler, B. M.; Schofield, C. J.; Davis, B. G. (2013). "DNA modification under mild conditions by Suzuki-Miyaura cross-coupling for the generation of functional probes". Angewandte Chemie International Edition. 52 (40): 10553–8. doi:10.1002/anie.201304038. PMC 3823066. PMID 23943570.
- ↑ Lin, Yuya Angel (2013). Olefin metathesis for site-selective protein modification (PhD thesis). University of Oxford.
- ↑ Patel, Little Kiran (2011). Unravelling the biological roles of charged carbohydrates (DPhil thesis). University of Oxford.
- ↑ Patel, M. K.; Davis, B. G. (2010). "Flow chemistry kinetic studies reveal reaction conditions for ready access to unsymmetrical trehalose analogues". Organic & Biomolecular Chemistry. 8 (19): 4232–5. doi:10.1039/c0ob00226g. PMID 20668770.
- ↑ Saliba, Regis C. (2014). Design and synthesis of nanoparticles functionalised with Lewis oligosaccharides for selective targeting of DC-SIGN (DPhil thesis). University of Oxford.
- ↑ Shanley, Samantha Jane (2009). A glycopore for bacterial sensing (DPhil thesis). University of Oxford.
- ↑ Wyszynski, Filip Jan (2010). Dissecting tunicamycin biosynthesis : a potent carbohydrate processing enzyme inhibitor (DPhil thesis). University of Oxford. OCLC 757140035.
- ↑ Wyszynski, F. J.; Lee, S. S.; Yabe, T; Wang, H; Gomez-Escribano, J. P.; Bibb, M. J.; Lee, S. J.; Davies, G. J.; Davis, B. G. (2012). "Biosynthesis of the tunicamycin antibiotics proceeds via unique exo-glycal intermediates". Nature Chemistry. 4 (7): 539–46. doi:10.1038/nchem.1351. PMID 22717438.
- ↑ Yamamoto, Keisuke (2013). Modification and application of glycosidases to create homogeneous glycoconjugates (DPhil thesis). University of Oxford.
- ↑ Yamamoto, K; Davis, B. G. (2012). "Creation of an α-mannosynthase from a broad glycosidase scaffold". Angewandte Chemie International Edition. 51 (30): 7449–53. doi:10.1002/anie.201201081. PMID 22696205.
- 1 2 3 "Professor Benjamin Davis FRS". London: The Royal Society. Archived from the original on 2 May 2015.
- 1 2 3 "Professor Benjamin Davis FRS". London: Royal Society. Archived from the original on 17 November 2015. One or more of the preceding sentences incorporates text from the royalsociety.org website where:
“All text published under the heading 'Biography' on Fellow profile pages is available under Creative Commons Attribution 4.0 International License.” --"Royal Society Terms, conditions and policies". Archived from the original on 25 September 2015. Retrieved 9 March 2016.
- ↑ Ben G. Davis's publications indexed by the Scopus bibliographic database, a service provided by Elsevier. (subscription required)
- ↑ Dixon, D. P.; Davis, B. G.; Edwards, R (2002). "Functional divergence in the glutathione transferase superfamily in plants. Identification of two classes with putative functions in redox homeostasis in Arabidopsis thaliana". Journal of Biological Chemistry. 277 (34): 30859–69. doi:10.1074/jbc.M202919200. PMID 12077129.
- ↑ Van Kasteren, S. I.; Kramer, H. B.; Jensen, H. H.; Campbell, S. J.; Kirkpatrick, J.; Oldham, N. J.; Anthony, D. C.; Davis, B. G. (2007). "Expanding the diversity of chemical protein modification allows post-translational mimicry". Nature. 446 (7139): 1105–9. doi:10.1038/nature05757. PMID 17460675.
- ↑ "Interview with Ben Davis: Sugar Solutions". Royal Society of Chemistry. Archived from the original on 2 June 2008.
- ↑ Robinson, M. A.; Charlton, S. T.; Garnier, P; Wang, X. T.; Davis, S. S.; Perkins, A. C.; Frier, M; Duncan, R; Savage, T. J.; Wyatt, D. A.; Watson, S. A.; Davis, B. G. (2004). "LEAPT: Lectin-directed enzyme-activated prodrug therapy". Proceedings of the National Academy of Sciences. 101 (40): 14527–32. doi:10.1073/pnas.0303574101. PMC 521935. PMID 15448212.