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Professor Massimo Hilliard
Professor

Massimo Hilliard

Email: 
Phone: 
+61 7 334 66390

Overview

Background

Queensland Brain Institute

Dr Massimo A. Hilliard received his PhD in Biological Chemistry and Molecular Biology in 2001 from the University of Naples, Italy. His experimental work, performed at the Institute of Genetics and Biophysics of the CNR (Italian National Council of Research), was aimed at understanding the neuronal and genetic basis of aversive taste behavior (bitter taste) in C. elegans.

During his first postdoc at the University of California, San Diego, using the Ca2+ indicator Cameleon he published the first direct visualisation of chemosensory activity in C. elegans neurons. In his second postdoctoral work at the University of California, San Francisco and at The Rockefeller University, he switched from neuronal function to neuronal development, focusing in particular on how neurons establish and orient their polarity with respect to extracellular cues.

From September 2007, he is at the Queensland Brain Institute where he established an independent laboratory.

Availability

Professor Massimo Hilliard is:
Available for supervision
Media expert

Fields of research

Qualifications

  • Bachelor of Science, Università degli Studi di Napoli Federico II
  • Doctor of Philosophy, Università degli Studi di Napoli Federico II

Research interests

  • Molecular and Cellular Neurobiology Laboratory

    We use C. elegans as a genetic model system to study neuronal development. There are currently three lines of research in the lab, and PhD projects and/or postdoctoral positions are available in each topic. 1. Axonal degeneration How neurons can maintain their axonal structure and function over time is not well understood. Axonal degeneration is a critical and common feature of many peripheral neuropathies, neurodegenerative diseases and nerve injuries. The genetic factors and the cellular mechanisms that prevent axonal degeneration under normal conditions and that trigger it under pathological ones are still largely unknown. We aim to use C. elegans genetics to identify the molecules and the mechanisms that control these processes. 2. Axonal regeneration How some axons can regenerate after nerve damage while others cannot is a crucial question in neurobiology, and the answers will be of great value for the medical handling of neurodegenerative diseases and of traumatic nerve injuries. Largely unknown are the molecules and the mechanisms underlying this important biological process. In C. elegans, a new laser-based technology allows single neuron axotomy in living animals, and axonal regeneration can now be visualised in real-time and tackled with a genetic approach. Our goal is to identify the genes and conditions that control this fascinating process. 3. Neuronal polarity and axonal guidance Neurons are highly polarized cells with distinct domains such as axons and dendrites. The polarity of a developing neuron determines the precise exit point of its axon as well as the initial trajectory of axon outgrowth. Understanding how neurons establish and orient polarity with respect to extracellular cues is an important and challenging problem in neurobiology. We wish to understand how different secreted cues regulate the orientation of neuronal polarity and axonal guidance in vivo.

Works

Search Professor Massimo Hilliard’s works on UQ eSpace

51 works between 1994 and 2025

21 - 40 of 51 works

2017

Journal Article

Phosphatidylserine save-me signals drive functional recovery of severed axons in Caenorhabditis elegans

Abay, Zehra C, Wong, Michelle Yu-Ying, Teoh, Jean-Sébastien, Vijayaraghavan, Tarika, Hilliard, Massimo A and Neumann, Brent (2017). Phosphatidylserine save-me signals drive functional recovery of severed axons in Caenorhabditis elegans. Proceedings of the National Academy of Sciences of the United States of America, 114 (47), 1-10. doi: 10.1073/pnas.1703807114

Phosphatidylserine save-me signals drive functional recovery of severed axons in Caenorhabditis elegans

2016

Journal Article

Cortical synaptic and dendritic spine abnormalities in a presymptomatic TDP-43 model of amyotrophic lateral sclerosis

Fogarty, Matthew J., Klenowski, Paul M., Lee, John D., Drieberg-Thompson, Joy R., Bartlett, Selena E., Ngo, Shyuan T., Hilliard, Massimo A., Bellingham, Mark C. and Noakes, Peter G. (2016). Cortical synaptic and dendritic spine abnormalities in a presymptomatic TDP-43 model of amyotrophic lateral sclerosis. Scientific Reports, 6 (1) 37968, 37968. doi: 10.1038/srep37968

Cortical synaptic and dendritic spine abnormalities in a presymptomatic TDP-43 model of amyotrophic lateral sclerosis

2016

Journal Article

Cell-cell fusion in the nervous system: alternative mechanisms of development, injury and repair

Giordano-Santini, Rosina, Linton, Casey and Hilliard, Massimo A. (2016). Cell-cell fusion in the nervous system: alternative mechanisms of development, injury and repair. Seminars in Cell and Developmental Biology, 60, 146-154. doi: 10.1016/j.semcdb.2016.06.019

Cell-cell fusion in the nervous system: alternative mechanisms of development, injury and repair

2016

Journal Article

Neuron-specific knock-down of SMN1 causes neuron degeneration and death through an apoptotic mechanism

Gallotta, Ivan, Mazzarella, Nadia, Donato, Alessandra, Esposito, Alessandro, Chaplin, Justin C., Castro, Silvana, Zampi, Giuseppina, Battaglia, Giorgio S., Hilliard, Massimo A., Bazzicalupo, Paolo and Di Schiavi, Elia (2016). Neuron-specific knock-down of SMN1 causes neuron degeneration and death through an apoptotic mechanism. Human Molecular Genetics, 25 (12), 2564-2577. doi: 10.1093/hmg/ddw119

Neuron-specific knock-down of SMN1 causes neuron degeneration and death through an apoptotic mechanism

2016

Journal Article

The apoptotic engulfment machinery regulates axonal degeneration in C. elegans neurons

Nichols, Annika L.A., Meelkop, Ellen, Linton, Casey, Giordano-Santini, Rosina, Sullivan, Robert K., Donato, Alessandra, Nolan, Cara, Hall, David H., Xue, Ding, Neumann, Brent and Hilliard, Massimo A. (2016). The apoptotic engulfment machinery regulates axonal degeneration in C. elegans neurons. Cell Reports, 14 (7), 1673-1683. doi: 10.1016/j.celrep.2016.01.050

The apoptotic engulfment machinery regulates axonal degeneration in C. elegans neurons

2015

Journal Article

EFF-1-mediated regenerative axonal fusion requires components of the apoptotic pathway

Neumann, Brent, Coakley, Sean, Giordano-Santini, Rosina, Linton, Casey, Lee, Eui Seung, Nakagawa, Akihisa, Xue, Ding and Hilliard, Massimo A. (2015). EFF-1-mediated regenerative axonal fusion requires components of the apoptotic pathway. Nature, 517 (7533), 219-222. doi: 10.1038/nature14102

EFF-1-mediated regenerative axonal fusion requires components of the apoptotic pathway

2014

Journal Article

A multi-channel device for high-density target-selective stimulation and long-term monitoring of cells and subcellular features in C. elegans

Lee, Hyewon, Kim, Shin Ae, Coakley, Sean, Mugno, Paula, Hammarlund, Marc, Hilliard, Massimo A. and Lu, Hang (2014). A multi-channel device for high-density target-selective stimulation and long-term monitoring of cells and subcellular features in C. elegans. Lab on a Chip - Miniaturisation for Chemistry and Biology, 14 (23), 4513-4522. doi: 10.1039/c4lc00789a

A multi-channel device for high-density target-selective stimulation and long-term monitoring of cells and subcellular features in C. elegans

2014

Journal Article

Loss of MEC-17 leads to microtubule instability and axonal degeneration

Neumann, Brent and Hilliard, Massimo A. (2014). Loss of MEC-17 leads to microtubule instability and axonal degeneration. Cell Reports, 6 (1), 93-103. doi: 10.1016/j.celrep.2013.12.004

Loss of MEC-17 leads to microtubule instability and axonal degeneration

2014

Conference Publication

High-throughput multichannel array device for selective stimulation and long-term in vivo imaging in C. elegans

Kim, Shin Ae, Lee, Hyewon, Hilliard, Massimo and Lu, Hang (2014). High-throughput multichannel array device for selective stimulation and long-term in vivo imaging in C. elegans. Food, Pharmaceutical and Bioengineering Division 2014 - Core Programming Area at the 2014 AIChE Annual Meeting, Atlanta GA, United States, 16-21 November 2014. American Institute of Chemical Engineers.

High-throughput multichannel array device for selective stimulation and long-term in vivo imaging in C. elegans

2013

Journal Article

Rapid and permanent neuronal inactivation in vivo via subcellular generation of reactive oxygen with the use of KillerRed

Williams, Daniel C., El Bejjani, Rachid, Mugno Ramirez, Paula, Coakley, Sean, Kim, Shin Ae, Lee, Hyewon, Wen, Quan, Samuel, Aravi, Lu, Hang, Hilliard, Massimo A. and Hammarlund, Marc (2013). Rapid and permanent neuronal inactivation in vivo via subcellular generation of reactive oxygen with the use of KillerRed. Cell Reports, 5 (2), 553-563. doi: 10.1016/j.celrep.2013.09.023

Rapid and permanent neuronal inactivation in vivo via subcellular generation of reactive oxygen with the use of KillerRed

2013

Journal Article

A dominant mutation in mec-7/β-tubulin affects axon development and regeneration in Caenorhabditis elegans neurons

Kirszenblat, Leonie, Neumann, Brent, Coakley, Sean and Massimo Hilliard (2013). A dominant mutation in mec-7/β-tubulin affects axon development and regeneration in Caenorhabditis elegans neurons. Molecular Biology of the Cell, 24 (3), 285-296. doi: 10.1091/mbc.E12-06-0441

A dominant mutation in mec-7/β-tubulin affects axon development and regeneration in Caenorhabditis elegans neurons

2012

Journal Article

A core metabolic enzyme mediates resistance to phosphine gas

Schlipalius, David I., Valmas, Nicholas, Tuck, Andrew G., Jagadeesan, Rajeswaran, Ma, Li, Kaur, Ramandeep, Goldinger, Anita, Anderson, Cameron, Kuang, Jujiao, Zuryn, Steven, Mau, Yosep S., Cheng, Qiang, Collins, Patrick J., Nayak, Manoj K., Schirra, Horst Joachim, Hilliard, Massimo A. and Ebert, Paul R. (2012). A core metabolic enzyme mediates resistance to phosphine gas. Science, 338 (6108), 807-810. doi: 10.1126/science.1224951

A core metabolic enzyme mediates resistance to phosphine gas

2012

Journal Article

Laterally orienting C. elegans using geometry at microscale for high-throughput visual screens in neurodegeneration and neuronal development studies

Cáceres, Ivan de Carlos, Valmas, Nicholas, Hilliard, Massimo A. and Lu, Hang (2012). Laterally orienting C. elegans using geometry at microscale for high-throughput visual screens in neurodegeneration and neuronal development studies. PLoS One, 7 (4) e35037, e35037.1-e35037.8. doi: 10.1371/journal.pone.0035037

Laterally orienting C. elegans using geometry at microscale for high-throughput visual screens in neurodegeneration and neuronal development studies

2012

Conference Publication

Fast target-selective chemical & optical stimulation based on high-throughput multi-channel imaging device

Lee, Hyewon, Kim, Shin Ae, Aubry, Guillaume, Mugno, Paula, Hilliard, Massimo and Lu, Hang (2012). Fast target-selective chemical & optical stimulation based on high-throughput multi-channel imaging device. 16th International Conference on Miniaturized Systems for Chemistry and Life Sciences, MicroTAS 2012, Okinawa, Japan, 28 October - 1 November 2012. San Diego, CA, United States: Chemical and Biological Microsystems Society.

Fast target-selective chemical & optical stimulation based on high-throughput multi-channel imaging device

2011

Journal Article

LIN-44/Wnt directs dendrite outgrowth through LIN-17/Frizzled in C. elegans neurons

Kirszenblat, Leonie, Pattabiraman, Divya and Hilliard, Massimo A. (2011). LIN-44/Wnt directs dendrite outgrowth through LIN-17/Frizzled in C. elegans neurons. PLoS Biology, 9 (9) e1001157, 0nline. doi: 10.1371/journal.pbio.1001157

LIN-44/Wnt directs dendrite outgrowth through LIN-17/Frizzled in C. elegans neurons

2011

Journal Article

Axonal regeneration proceeds through specific axonal fusion in transected C. elegans neurons

Neumann, Brent, Nguyen, Ken C. Q., Hall, David H., Ben-Yakar, Adela and Hilliard, Massimo A. (2011). Axonal regeneration proceeds through specific axonal fusion in transected C. elegans neurons. Developmental Dynamics, 240 (6), 1365-1372. doi: 10.1002/dvdy.22606

Axonal regeneration proceeds through specific axonal fusion in transected C. elegans neurons

2011

Journal Article

Big ideas for small brains: What can psychiatry learn from worms, flies, bees and fish?

Burne, T. H. J., Scott, E., van Swinderen, B., Hilliard, M., Reinhard, J., Claudianos, C., Eyles, D. W. and McGrath, J. J. (2011). Big ideas for small brains: What can psychiatry learn from worms, flies, bees and fish?. Molecular Psychiatry, 16 (1), 7-16. doi: 10.1038/mp.2010.35

Big ideas for small brains: What can psychiatry learn from worms, flies, bees and fish?

2009

Journal Article

Axonal degeneration and regeneration: a mechanistic tug-of-war

Hilliard, Massimo (2009). Axonal degeneration and regeneration: a mechanistic tug-of-war. Journal Of Neurochemistry, 108 (1), 23-32. doi: 10.1111/j.1471-4159.2008.05754.x

Axonal degeneration and regeneration: a mechanistic tug-of-war

2008

Conference Publication

Femtosecond laser nanosurgery in microfluidic devices and its emerging role in nerve regeneration studies

Guo, Samuel X., Bourgeois, Frederic, Chokshi, Trushal, Durr, Nicholas J., Hilliard, Massimo, Chronis, Nikos and Ben-Yakar, Adela (2008). Femtosecond laser nanosurgery in microfluidic devices and its emerging role in nerve regeneration studies. doi: 10.1109/LEOS.2008.4688576

Femtosecond laser nanosurgery in microfluidic devices and its emerging role in nerve regeneration studies

2008

Journal Article

Femtosecond laser nanoaxotomy lab-on-a-chip for in vivo nerve regeneration studies

Guo, Samuel X., Bourgeois, Frederic, Chokshi, Trushal, Durr, Nicholas J., Hilliard, Massimo A., Chronis, Nikos and Ben-Yakar, Adela (2008). Femtosecond laser nanoaxotomy lab-on-a-chip for in vivo nerve regeneration studies. Nature Methods, 5 (6), 531-533. doi: 10.1038/nmeth.1203

Femtosecond laser nanoaxotomy lab-on-a-chip for in vivo nerve regeneration studies

Funding

Current funding

  • 2025 - 2027
    Understanding neuronal fusion in nervous system development and remodelling
    ARC Discovery Projects
    Open grant
  • 2021 - 2025
    Axonal regeneration and degeneration: cellular and molecular mechanisms
    NHMRC Investigator Grants
    Open grant

Past funding

  • 2021 - 2024
    The Australian Functional Genomics Network (Administered by Murdoch Children's Research Institute)
    Murdoch Childrens Research Institute
    Open grant
  • 2019 - 2022
    Understanding the role of the metalloprotease ADM-4/ADAM17/TACE in promoting axonal repair
    NHMRC Project Grant
    Open grant
  • 2019 - 2022
    Understanding the role of UNC-71 in axonal regeneration.
    NHMRC Project Grant
    Open grant
  • 2018
    A multifunctional platform for monitoring and manipulating neural activities with freely behaving small animals
    NHMRC Equipment Grant
    Open grant
  • 2018 - 2022
    Identification and study of novel conserved molecule with an axonal protective function
    NHMRC Project Grant
    Open grant
  • 2017
    Lattice light sheet microscopy for imaging biology in real space and time
    ARC Linkage Infrastructure, Equipment and Facilities
    Open grant
  • 2017 - 2019
    Epigenetic determination of neuronal vulnerability and neurodegenerative disease
    NHMRC Project Grant
    Open grant
  • 2017 - 2020
    Understanding axonal fusion: an alternative mechanism to repair injured axons.
    NHMRC Project Grant
    Open grant
  • 2016
    A state-of-the-art facility for simulataneous photo-stimulation, high speed imaging and electrophysiological recording of multiple neurons in brain tissue and living organisms
    UQ Major Equipment and Infrastructure
    Open grant
  • 2016
    Automatic plate pourer
    NHMRC Equipment Grant
    Open grant
  • 2016
    Axonal Fusion: New strategies to repair injured axons
    Vice-Chancellor's Research Focused Fellowship
    Open grant
  • 2016 - 2020
    Axonal regeneration and degeneration: cellular and molecular mechanisms
    NHMRC Research Fellowship
    Open grant
  • 2016 - 2018
    The role of membrane phospholipids in regenerative axonal fusion (NHMRC Project Grant administered by Monash University)
    Monash University
    Open grant
  • 2016 - 2020
    Understanding the molecular mechanisms regulating neuronal fusion.
    ARC Discovery Projects
    Open grant
  • 2015
    Computerised stereotaxic stages and rapid tissue processor for enhanced fixation and immunolabelling
    NHMRC Equipment Grant
    Open grant
  • 2015
    Spectral Applied Research spinning disc confocal microscope for high speed 3D imaging of tissue and live organisms
    UQ Major Equipment and Infrastructure
    Open grant
  • 2014 - 2017
    Axonal fusion to promote nerve repair: molecules and mechanisms.
    NHMRC Project Grant
    Open grant
  • 2014 - 2016
    Understanding the role of TDP-43 in motor neuron disease.
    NHMRC Project Grant
    Open grant
  • 2013
    Spinning disk confocal for advanced high-speed histocytometry and neuromorphology analysis
    UQ Major Equipment and Infrastructure
    Open grant
  • 2012
    Analysis of TDP-43 Target genes in C. elegans
    Motor Neurone Disease Research Institute of Australia Inc
    Open grant
  • 2012 - 2015
    Molecules and mechanisms regulating axonal degeneration and regeneration in C. elegans neurons
    ARC Future Fellowships
    Open grant
  • 2011
    An automated liquid handling platform for High-throughput Preparation of multiplexed targeted sequence capture DNA libraries for Next-Generation DNA Sequencing (NGS)
    UQ Major Equipment and Infrastructure
    Open grant
  • 2010 - 2011
    Molecular Mechanisms of Axonal Regeneration in C. elegans Neurons
    UQ Foundation Research Excellence Awards - DVC(R) Funding
    Open grant
  • 2010 - 2012
    Discovering molecules and mechanisms regulating dendrite formation
    NHMRC Project Grant
    Open grant
  • 2010 - 2012
    Membrane fusion in axonal regeneration: molecules and mechanisms
    NHMRC Project Grant
    Open grant
  • 2010
    Next-generation DNA sequencer to accelerate discovery in molecular and cellular research programs at QBI
    UQ Major Equipment and Infrastructure
    Open grant
  • 2009 - 2011
    Axonal degeneration in C. elegans neurons
    NHMRC Project Grant
    Open grant
  • 2008 - 2011
    Femtosecond laser axotomy for in vivo nerve regeneration studies in C. elegans.
    University of Texas at Austin - Grants
    Open grant

Supervision

Availability

Professor Massimo Hilliard is:
Available for supervision

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

Supervision history

Current supervision

  • Doctor Philosophy

    Investigating the role of oxidative stress in neurodegeneration.

    Principal Advisor

    Other advisors: Associate Professor Steven Zuryn

  • Doctor Philosophy

    Axonal degeneration and regeneration in C. elegans neurons

    Principal Advisor

    Other advisors: Dr Sean Coakley

  • Doctor Philosophy

    Molecular pathway elucidation of TDP-43 pathology

    Associate Advisor

    Other advisors: Associate Professor Adam Walker

  • Doctor Philosophy

    Molecular elucidation of TDP-43 co-aggregators in models of ALS/FTD

    Associate Advisor

    Other advisors: Associate Professor Adam Walker

  • Doctor Philosophy

    Determining how mitochondrial quality is maintained within axons

    Associate Advisor

    Other advisors: Associate Professor Steven Zuryn

  • Doctor Philosophy

    Molecular elucidation of TDP-43 co-aggregators in models of ALS/FTD

    Associate Advisor

    Other advisors: Associate Professor Adam Walker

Completed supervision

Media

Enquiries

Contact Professor Massimo Hilliard directly for media enquiries about:

  • Axonal degeneration
  • Brain - regeneration
  • Brain conditions
  • Brain degeneration
  • C. elegans
  • Degeneration - brain
  • Dendrite outgrowth
  • Diseases - neurodegenerative
  • Genetics - neuroscience
  • Imaging - brain
  • Molecular biology
  • Nerve injury
  • Neurodegenerative diseases
  • Neuronal development
  • Neuronal polarity
  • Neuroscience
  • Regeneration - brain

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