Professor Alan Mark
Professor

Alan Mark

Email: 

Background

We use computer based modelling techniques to understand and predict the the structural and dynamic properties of (bio)molecules including proteins and lipid aggregates.

Born in 1961, I obtained a BSc (Hon 1) at the University of Sydney in 1982. I obtained my PhD in 1986 from the John Curtin School of Medical Research, Australian National University (ANU), on the "Binding Responses Associated with Self-Interacting Ligands: Studies on the Self-Association and Receptor binding of Insulin”. After holding postdoctoral positions at the ANU, University of Groningen, The Netherlands and the Federal Institute of Technology (ETH), Zurich, Switzerland I was appointed Professor of Biophysical Chemistry (Molecular Simulation) University of Groningen, in 1998. In 1998 I also received the Swiss Ruzicka Prize for research in Chemistry for work on simulating peptide folding. In 2004 I was awarded an ARC Federation Fellowship and in February 2005 an honorary chair (Bijzonder Hoogleraar) at the University of Groningen, The Netherlands. I have given over 90 invited lectures at conferences and academic Institutions around the world as well as at a range of summer and winter schools on advanced simulation techniques.

In my research I have performed pioneering simulations of a variety of important biological phenomena, including some of the first atomic simulations of protein unfolding and the first simulations of reversible peptide folding in a realistic environment. In recent years my group performed some of the first atomic and near atomic simulations of the spontaneous aggregation of surfactant and lipid systems into micelles, bilayers and vesicles. These have enabled us, amongst other things, to elucidate the mechanism by which pores are induced within biological membranes in unprecedented detail. Over the last decade I have been intimately involved in the development of the GROMOS force field which is specifically tuned for protein and peptide folding simulations and as well as the development of models for a range of solvents including methanol and trifluoroethanol. I have also been responsible for the development of methodology for the calculations of the thermodynamic properties of biomolecular systems such as free energies of binding and hydration, as well as estimating entropic effects from simulations. Most recently, I have been responsible for the development of novel approaches to promote structure formation in protein folding simulations that can be used for the refinement of protein structures generated by ab initio or by homology methods. Finally, I am associated with two, internationally recognised, (bio)molecular simulation packages the GROningen Molecular Simulation library (GROMOS) and the GROningen Machine for Chemical Simulations (GROMACS).

Availability

Professor Alan Mark is:
Available for supervision
Media expert

Fields of research

Chemical Sciences

Qualifications

  • Bachelor (Honours) of Science (Advanced), University of Sydney
  • Doctor of Philosophy, Australian National University

Search Professor Alan Mark’s works on UQ eSpace

257 works between 1984 and 2024
All (257) Journal Article (226) Book Chapter (3) Conference Publication (27) Other Outputs (1)

41 - 60 of 257 works

2017

Conference Publication

Enumerating common molecular substructures

Engler, Martin S., El-Kebir, Mohammed, Mulder, Jelmer, Mark, Alan E., Geerke, Daan P. and Klau, Gunnar W. (2017). Enumerating common molecular substructures. German Conference on Bioinformatics, GCB 2017, Tubingen, Germany, 18-21 September 2017. Tubingen, Germany: Gesellschaft fur Informatik. doi: 10.7287/peerj.preprints.3250v1

Enumerating common molecular substructures

2016

Journal Article

The CC domain structure from the wheat stem rust resistance protein Sr33 challenges paradigms for dimerization in plant NLR proteins

Casey, Lachlan W., Lavrencic, Peter, Bentham, Adam R., Cesari, Stella, Ericsson, Daniel J., Croll, Tristan, Turk, Dušan, Anderson, Peter A., Mark, Alan E., Dodds, Peter N., Mobli, Mehdi, Kobe, Bostjan and Williams, Simon J. (2016). The CC domain structure from the wheat stem rust resistance protein Sr33 challenges paradigms for dimerization in plant NLR proteins. Proceedings of the National Academy of Sciences, 113 (45), 12856-12861. doi: 10.1073/pnas.1609922113

The CC domain structure from the wheat stem rust resistance protein Sr33 challenges paradigms for dimerization in plant NLR proteins

2016

Journal Article

Deriving structural information from experimentally measured data on biomolecules

van Gunsteren, Wilfred F., Allison, Jane R., Daura, Xavier, Dolenc, Jožica, Hansen, Niels, Mark, Alan E., Oostenbrink, Chris, Rusu, Victor H. and Smith, Lorna J. (2016). Deriving structural information from experimentally measured data on biomolecules. Angewandte Chemie International Edition, 55 (52), 15990-16010. doi: 10.1002/anie.201601828

Deriving structural information from experimentally measured data on biomolecules

2016

Journal Article

Bestimmung von strukturinformation aus experimentellen messdaten für biomoleküle

van Gunsteren, Wilfred F., Allison, Jane R., Daura, Xavier, Dolenc, Jožica, Hansen, Niels, Mark, Alan E., Oostenbrink, Chris, Rusu, Victor H. and Smith, Lorna J. (2016). Bestimmung von strukturinformation aus experimentellen messdaten für biomoleküle. Angewandte Chemie, 128 (52), 16222-16244. doi: 10.1002/ange.201601828

Bestimmung von strukturinformation aus experimentellen messdaten für biomoleküle

2016

Journal Article

Interaction of tarantula venom peptide ProTx-II with lipid membranes is a prerequisite for its inhibition of human voltage-gated sodium channel NaV1.7

Troeira Henriques, Sonia, Deplazes, Evelyne, Lawrence, Nicole, Cheneval, Olivier, Chaousis, Stephanie, Inserra, Marco, Thongyoo, Panumart, King, Glenn F., Mark, Alan E., Vetter, Irina, Craik, David J. and Schroeder, Christina Ingrid (2016). Interaction of tarantula venom peptide ProTx-II with lipid membranes is a prerequisite for its inhibition of human voltage-gated sodium channel NaV1.7. The Journal of Biological Chemistry, 291 (33), 17049-17065. doi: 10.1074/jbc.M116.729095

Interaction of tarantula venom peptide ProTx-II with lipid membranes is a prerequisite for its inhibition of human voltage-gated sodium channel NaV1.7

2016

Journal Article

Revisiting the scissor-like mechanism of activation for the erythropoietin receptor

Corbett, Michael S. P., Poger, David and Mark, Alan E. (2016). Revisiting the scissor-like mechanism of activation for the erythropoietin receptor. FEBS Letters, 590 (18), 3083-3088. doi: 10.1002/1873-3468.12340

Revisiting the scissor-like mechanism of activation for the erythropoietin receptor

2016

Journal Article

Outcome of the first wwPDB/CCDC/D3R ligand validation workshop

Adams, Paul D., Aertgeerts, Kathleen, Bauer, Cary, Bell, Jeffrey A., Berman, Helen M., Bhat, Talapady N., Blaney, Jeff M., Bolton, Evan, Bricogne, Gerard, Brown, David, Burley, Stephen K., Case, David A., Clark, Kirk L., Darden, Tom, Emsley, Paul, Feher, Victoria A., Feng, Zukang, Groom, Colin R., Harris, Seth F., Hendle, Jorg, Holder, Thomas, Joachimiak, Andrzej, Kleywegt, Gerard J., Krojer, Tobias, Marcotrigiano, Joseph, Mark, Alan E., Markley, John L., Miller, Matthew, Minor, Wladek ... Young, Jasmine (2016). Outcome of the first wwPDB/CCDC/D3R ligand validation workshop. Structure, 24 (4), 502-508. doi: 10.1016/j.str.2016.02.017

Outcome of the first wwPDB/CCDC/D3R ligand validation workshop

2016

Journal Article

Understanding the accumulation of P-glycoprotein substrates within cells: The effect of cholesterol on membrane partitioning

Subramanian, Nandhitha, Schumann-Gillett, Alexandra, Mark, Alan E. and O'Mara, Megan L. (2016). Understanding the accumulation of P-glycoprotein substrates within cells: The effect of cholesterol on membrane partitioning. Biochimica et Biophysica Acta: Biomembranes, 1858 (4), 776-782. doi: 10.1016/j.bbamem.2015.12.025

Understanding the accumulation of P-glycoprotein substrates within cells: The effect of cholesterol on membrane partitioning

2016

Journal Article

Validating lipid force fields against experimental data: progress, challenges and perspectives.

Poger, David, Caron, Bertrand and Mark, Alan E. (2016). Validating lipid force fields against experimental data: progress, challenges and perspectives.. Biochimica et Biophysica Acta, 1858 (7), 1556-1565. doi: 10.1016/j.bbamem.2016.01.029

Validating lipid force fields against experimental data: progress, challenges and perspectives.

2016

Journal Article

Membrane-binding properties of gating modifier and pore-blocking toxins: membrane interaction is not a prerequisite for modification of channel gating

Deplazes, Evelyne, Troeira Henriques, Sonia, Smith, Jennifer J., King, Glenn F., Craik, David J., Mark, Alan E. and Schroeder, Christina I. (2016). Membrane-binding properties of gating modifier and pore-blocking toxins: membrane interaction is not a prerequisite for modification of channel gating. Biochimica et Biophysica Acta - Biomembranes, 1858 (4), 872-882. doi: 10.1016/j.bbamem.2016.02.002

Membrane-binding properties of gating modifier and pore-blocking toxins: membrane interaction is not a prerequisite for modification of channel gating

2016

Conference Publication

Going downstream - how does GH binding activate JAK2

Brooks, Andrew, Dai, W., O'Mara, M. L., Abankwa, D., Chhabra, Y., Pelekanos, R. A., Gardon, O., Tunny, K. A., Blucher, K. M., Morton, C. J., Parker, M. W., Sierecki, E., Gambin, Y., Gomez, G. A., Alexandrov, K., Wilson, I. A., Doxastakis, M., Mark, A. E. and Waters, M. J. (2016). Going downstream - how does GH binding activate JAK2. Annual Scientific Meeting of the Endocrine Society of Australia, Adelaide, Australia, 23-26 August, 2015. Chichester, West Sussex, United Kingdom: Wiley-Blackwell Publishing. doi: 10.1111/cen.13010

Going downstream - how does GH binding activate JAK2

2016

Conference Publication

A cytokine receptor revolution: activation of the Type-I Cytokine Receptors via protomer rotation

Corbett, Michael, Poger, David and Mark, Alan E. (2016). A cytokine receptor revolution: activation of the Type-I Cytokine Receptors via protomer rotation. 60th Annual Meeting of the Biophysical Society, Los Angeles, CA, United States, 27 February- 2 March 2016. St. Louis, MO, United States: Cell Press. doi: 10.1016/j.bpj.2015.11.3161

A cytokine receptor revolution: activation of the Type-I Cytokine Receptors via protomer rotation

2016

Journal Article

Combination of Ambiguous and Unambiguous Data in the Restraint-driven Docking of Flexible Peptides with HADDOCK: The Binding of the Spider Toxin PcTx1 to the Acid Sensing Ion Channel (ASIC) 1a

Deplazes, Evelyne, Davies, Josephine, Bonvin, Alexandre M. J. J., King, Glenn F. and Mark, Alan E. (2016). Combination of Ambiguous and Unambiguous Data in the Restraint-driven Docking of Flexible Peptides with HADDOCK: The Binding of the Spider Toxin PcTx1 to the Acid Sensing Ion Channel (ASIC) 1a. Journal of Chemical Information and Modeling, 56 (1), 127-138. doi: 10.1021/acs.jcim.5b00529

Combination of Ambiguous and Unambiguous Data in the Restraint-driven Docking of Flexible Peptides with HADDOCK: The Binding of the Spider Toxin PcTx1 to the Acid Sensing Ion Channel (ASIC) 1a

2016

Conference Publication

On the Combination of Restraint-Driven Docking of Flexible Peptides to Ion Channels - Lessons Learnt from the Complex Formed by the Spider Venom PcTx1 and the Acid Sensing Ion Channel1

Deplazes, Evelyne, Davies, Josephine, Bonvin, Alexandre M. J. J. and Mark, Alan E. (2016). On the Combination of Restraint-Driven Docking of Flexible Peptides to Ion Channels - Lessons Learnt from the Complex Formed by the Spider Venom PcTx1 and the Acid Sensing Ion Channel1. 60th Annual Meeting of the Biophysical-Society, Los Angeles, CA, United States, February 27- March 2 2016. St Louis, United States: Cell Press. doi: 10.1016/j.bpj.2015.11.2872

On the Combination of Restraint-Driven Docking of Flexible Peptides to Ion Channels - Lessons Learnt from the Complex Formed by the Spider Venom PcTx1 and the Acid Sensing Ion Channel1

2016

Conference Publication

Membrane-binding properties of gating-modifier and pore blocking toxins: membrane interaction is not a prerequisite for modification of channel gating

Deplazes, Evelyne, Henriques, Sonia Troeira, King, Glenn F., Craik, David J., Mark, Alan E. and Schroeder, Christina I. (2016). Membrane-binding properties of gating-modifier and pore blocking toxins: membrane interaction is not a prerequisite for modification of channel gating. 60th Annual Meeting of the Biophysical-Society, Los Angeles, United States, February 27- March 2 2016. St Louis, United States: Cell Press. doi: 10.1016/j.bpj.2015.11.220

Membrane-binding properties of gating-modifier and pore blocking toxins: membrane interaction is not a prerequisite for modification of channel gating

2016

Conference Publication

Mechanism of JAK2 Activation by the Archetype Class I Cytokine Receptor, the Growth Hormone Receptor

Brooks, Andrew J., O’Mara, Megan L., Dai, Wei, Abankwa, Daniel, Chhabra, Yash, Tunny, Kathryn A., Parker, Michael W., Sierecki, Emma, Gambin, Yann, Gomez, Guillermo A., Haxholm, Gitte W., Nikolajsen, Louise F., Doxastakis, Manolis, Mark, Alan E. and Waters, Michael J. (2016). Mechanism of JAK2 Activation by the Archetype Class I Cytokine Receptor, the Growth Hormone Receptor. Biophysical Meeting, Los Angeles, CA, United States, 27 February - 2 March 2016. CAMBRIDGE: CELL PRESS. doi: 10.1016/j.bpj.2015.11.233

Mechanism of JAK2 Activation by the Archetype Class I Cytokine Receptor, the Growth Hormone Receptor

2015

Journal Article

Effect of Ring Size in ω-Alicyclic Fatty Acids on the Structural and Dynamical Properties Associated with Fluidity in Lipid Bilayers

Poger, David and Mark, Alan E. (2015). Effect of Ring Size in ω-Alicyclic Fatty Acids on the Structural and Dynamical Properties Associated with Fluidity in Lipid Bilayers. Langmuir, 31 (42), 11574-11582. doi: 10.1021/acs.langmuir.5b02635

Effect of Ring Size in ω-Alicyclic Fatty Acids on the Structural and Dynamical Properties Associated with Fluidity in Lipid Bilayers

2015

Journal Article

Molecular dynamics and functional studies define a hot spot of crystal contacts essential for PcTx1 inhibition of acid-sensing ion channel 1a

Saez, Natalie J., Deplazes, Evelyne, Cristofori-Armstrong, Ben, Chassagnon, Irene R., Lin, Xiaozhen, Mobli, Mehdi, Mark, Alan E., Rash, Lachlan D. and King, Glenn F. (2015). Molecular dynamics and functional studies define a hot spot of crystal contacts essential for PcTx1 inhibition of acid-sensing ion channel 1a. British Journal of Pharmacology, 172 (20), 4985-4995. doi: 10.1111/bph.13267

Molecular dynamics and functional studies define a hot spot of crystal contacts essential for PcTx1 inhibition of acid-sensing ion channel 1a

2015

Journal Article

Binding of starch fragments to the starch branching enzyme: implications for developing slower-digesting starch

Go, Rob Marc, Mark, Alan E., Malde, Alpeshkumar K. and Gilbert, Robert G. (2015). Binding of starch fragments to the starch branching enzyme: implications for developing slower-digesting starch. Biomacromolecules, 16 (8), 2475-2481. doi: 10.1021/acs.biomac.5b00710

Binding of starch fragments to the starch branching enzyme: implications for developing slower-digesting starch

2015

Journal Article

Identification of possible binding sites for morphine and nicardipine on the multidrug transporter P-Glycoprotein using umbrella sampling techniques

Subramanian, Nandhitha, Condic-Jurkic, Karmen, Mark, Alan E. and O'Mara, Megan L. (2015). Identification of possible binding sites for morphine and nicardipine on the multidrug transporter P-Glycoprotein using umbrella sampling techniques. Journal of Chemical Information and Modeling, 55 (6), 1202-1217. doi: 10.1021/ci5007382

Identification of possible binding sites for morphine and nicardipine on the multidrug transporter P-Glycoprotein using umbrella sampling techniques

Current funding

  • 2023 - 2030
    ARC Centre of Excellence in Quantum Biotechnology
    ARC Centres of Excellence
    Open grant
  • 2023 - 2025
    CRACing the role of the Flavivirus NS1 protein
    NHMRC IDEAS Grants
    Open grant
  • 2022 - 2025
    Validation of predicted solution processed organic semiconductor properties
    ARC Discovery Projects
    Open grant

Past funding

  • 2022 - 2025
    Enhanced force fields for computational drug design and materials research.
    ARC Discovery Projects
    Open grant
  • 2020 - 2022
    Elucidating the morphology of organic semiconductors at an atomic level
    ARC Linkage Projects
    Open grant
  • 2019 - 2022
    Sustaining and enhancing merit-based research access to the National Computational Infrastructure (ARC LIEF project administered by ANU)
    Australian National University
    Open grant
  • 2019
    Expanding Wiener, a high performance GPU cluster
    UQ Research Facilities Infrastructure Grants
    Open grant
  • 2018 - 2021
    Improving empirical force fields: A big-data approach
    ARC Discovery Projects
    Open grant
  • 2016 - 2019
    From molecules to cells: understanding the structural and dynamic properties of cellular components at an atomic level
    UQ Fellowships
    Open grant
  • 2016 - 2018
    Maintaining and enhancing merit-based access to the NCI National Facility (ARC LIEF project administered by The Australian National University)
    Australian National University
    Open grant
  • 2016 - 2018
    Understanding biological membranes in atomic detail
    ARC Discovery Projects
    Open grant
  • 2015 - 2020
    Autotyping of United Atom Force Field Parameters
    The Procter & Gamble Co.
    Open grant
  • 2015 - 2018
    A New Paradigm for Class I Cytokine Receptor Activation
    NHMRC Project Grant
    Open grant
  • 2015 - 2017
    Force Fields for Structure Refinement and Computational Drug Design
    ARC Discovery Projects
    Open grant
  • 2014
    A parallel computer facility for modelling and simulation
    UQ Major Equipment and Infrastructure
    Open grant
  • 2013 - 2015
    Membrane proteins: Understanding biological switches, motors and triggers.
    ARC Discovery Projects
    Open grant
  • 2013 - 2015
    Selective targeting of microbes by peptides of the innate immune system
    NHMRC Project Grant
    Open grant
  • 2013 - 2016
    Understanding multidrug resistance in cancer: identification of the substrate and inhibitor binding sites in P-glycoprotein
    NHMRC Project Grant
    Open grant
  • 2012 - 2015
    Strengthening merit-based access and support at the new National Computing Infrastructure petascale supercomputing facility (ARC LIEF Grant administered by ANU)
    ARC LIEF Collaborating/Partner Organisation Contributions
    Open grant
  • 2012 - 2014
    Structural biology of bacterial lipid II-glycopeptide antibiotic interactions
    NHMRC Project Grant
    Open grant
  • 2011 - 2013
    Development of potent and selective blockers of acid sensing ion channels for the treatment of pain
    NHMRC Project Grant
    Open grant
  • 2011
    GO8 - 2011 European Fellowships - Dr Larisa Zoranic: The action of anti-microbial peptides
    Group of Eight European Fellowship
    Open grant
  • 2011 - 2017
    Understanding sub-cellular systems at the atomic level
    Vice-Chancellor's Senior Research Fellowship
    Open grant
  • 2011 - 2013
    Understanding sub-cellular systems at the atomic level
    ARC Discovery Projects
    Open grant
  • 2009 - 2011
    Development of cryopreservation for high value provenance collections of recalcitrant plant species used in post-mining restoration
    Curtin University of Technology
    Open grant
  • 2008 - 2009
    A computational facility for multi-scale modelling in bio and nanotechnology
    ARC Linkage Infrastructure, Equipment and Facilities
    Open grant
  • 2008 - 2010
    From structures to systems: A hierachical approach to understanding sub-cellular components.
    ARC Discovery Projects
    Open grant
  • 2008 - 2010
    Increasing the efficiency of biomolecular simulations
    ARC Linkage International
    Open grant
  • 2008 - 2010
    Molecular characterization of dengue virus fusion and antiviral inhibitors
    NHMRC Project Grant
    Open grant
  • 2007 - 2009
    Dynamic modelling of biomolecular systems: Going beyond classical empirical force fields.
    ARC Discovery Projects
    Open grant
  • 2005 - 2010
    Self Organisation In (Bio) Molecular Systems: Simulating The Folding And Aggregation Of Peptides, Proteins And Lipids
    ARC Federation Fellowships
    Open grant

Availability

Professor Alan Mark is:
Available for supervision

Before you email them, read our advice on how to contact a supervisor.

Available projects

  • Understanding the mechanism of action of antimicrobial peptides

    Cytolytic antimicrobial peptides form an integral part of the innate immune system of many vertebrates including man. These antimicrobial peptides act by binding to and disrupting bacterial cell membrane. They are highly specific and increasingly recognized as a potential source of novel antibiotic agents. A major limitation in the further development of AMPs in a therapeutic setting is that the mechanism by which these peptides discriminate between different classes of membranes is still poorly understood. The aim of this project is to use computer simulation techniques elucidate the mechanism of action of cytolytic peptides at an atomic level. Specifically to study their binding to the outer membrane of specific pathogenic bacteria and determine the key structural and physico-chemical properties that allows them to distinguish between the pathogenic intruder and host cells.

  • Force fields for drug-like molecules

    A critical consideration when modelling biomolecular systems is the description of the interactions. The aim of this project is to develop and validate an automated force field topology builder (ATB; http://compbio.biosci.uq.edu.au/atb/). The ATB provides force field descriptions for drug-like molecules for use in studying the ligand-macromolecule interactions with applications in drug design and X-ray refinement.

  • From model systems to true biological membranes

    Lipid molecules are fundamental components of biological membranes. Not only do they play a role in the compartmentalization of cells and organelles but, also participate in fundamental processes such as cell division and intracellular trafficking. The aim of this project is to develop detailed models representing the membranes of specific cell types.

  • The mechanism of activation of cytokine receptors:

    The activation of cell surface receptors such as the growth hormone receptor and the epidermal growth factor receptor is a critical step in cell regulation. Molecular dynamics simulation techniques will be used to characterize the conformational changes within the extracellular and transmembrane domains that accompany the binding of the cytokine (growth hormone1 or epidermal growth factor) to its receptor thereby shedding light on the mechanism of action of cytokine receptors in general.

Supervision history

Current supervision

  • Doctor Philosophy

    Enhanced force fields for computational drug design and materials research.

    Principal Advisor

    Other advisors: Professor Paul Burn

  • Doctor Philosophy

    Development of novel computational algorithms for biotechnological applications including molecular simulation and drug design

    Principal Advisor

  • Doctor Philosophy

    Investigation of pH-dependent bacterial transporters

    Principal Advisor

    Other advisors: Professor Debra Bernhardt

  • Doctor Philosophy

    Developing transferable force fields to simulate biological membranes

    Principal Advisor

  • Doctor Philosophy

    Validation of predicted solution processed organic semiconductor properties

    Associate Advisor

    Other advisors: Associate Professor Paul Shaw, Professor Paul Burn

Completed supervision

Enquiries

Contact Professor Alan Mark directly for media enquiries about:

  • Atomic force fields
  • Computational drug design
  • Computer simulation - molecular
  • Drug design
  • Free energy calculations
  • GROMACS - GROningen MAchine for Chemical Simulations
  • GROMOS - force field for molecular dynamics simulation
  • Molecular dynamics
  • Molecules and computation
  • Protein folding
  • Protein structure

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