Professor Michael Piper
Professor

Michael Piper

Email: 
Phone: 
+61 7 334 69873

Background

I graduated from The University of Tasmania, and received my PhD in Developmental Biology from The University of Queensland in 2003. My PhD, performed at the Institute for Molecular Bioscience with Prof. Melissa Little, centred on understanding the cellular and molecular mechanisms underlying embryonic kidney development. My first postdoc was performed with Prof. Christine Holt at The University of Cambridge, UK, where I studied the mechanisms by which axonal growth cones navigate to their targets in the brain, using the frog Xenopus laevis as a model system. In my second postdoctoral position, with Prof. Linda Richards at the Queensland Brain Institute at The University of Queensland, my work focussed on understanding the molecular mechanisms of neural progenitor cell specification in the developing cerebral cortex. In late 2010, I took up a joint position with the Queensland Brain Institute and The School of Biomedical Sciences (SBMS) to continue my research into the mechanisms underlying neural stem cell differentiation. I have held numerous fellowships during my career, including an NHMRC Howard Florey Fellowship, an NHMRC CDF and an ARC Future Fellowship. I currently hold a continuing Teaching and Research position within SBMS, and am currently the Director for Higher Degree Research Training at SBMS.

Availability

Professor Michael Piper is:
Available for supervision

Fields of research

Biological Sciences Biomedical and Clinical Sciences Cell and nuclear division Cellular nervous system Epigenetics (incl. genome methylation and epigenomics) Genetics Neurosciences

Qualifications

  • Bachelor (Honours) of Science (Advanced), University of Tasmania
  • Doctor of Philosophy, The University of Queensland

Research interests

  • Understanding the drivers of neural stem cell differentiation

    What are the mechanisms that control neural stem cell (NSC) differentiation during embryogenesis, and that enable the generation of the diverse suite of neurons and glia that comprise the brain? This is a key question in developmental neuroscience. My contribution to this field to date has been to reveal central transcriptional regulators that mediate NSC biology within the brain. Using rodent model systems, I demonstrated that transcription factors of the Nuclear Factor One (NFI) family mediate NSC proliferation and differentiation in the embryonic, postnatal and adult nervous system. This work has received international recognition, as evidenced by numerous invited international presentations and high-impact reviews (e.g. Trends in Cell Biology), and forms the framework around which the hypotheses of this program will be addressed. I am interested in defining how NSC proliferation and differentiation is regulated at a transcriptional and epigenomic level within the developing nervous system. Using the developing mouse brain as a model system, we are using a suite of molecular and cellular techniques to understand how diverse regions of the nervous system are generated, including the cerebral cortex, the cerebellum, the spinal cord and the hypothalamus. For example, within the cerebral cortex, we are investigating how the NFI family of transcription factors mediate NSC differentiation, and how mutations to the NFI family culminate in macrocephaly, and disorders such as Malan syndrome. Moreover, we are using mice lacking the gene Nsd1 (a histone modifying protein) to investigate the development of a human syndrome known as Sotos syndrome, which is also characterised by macrocephaly. In collaboration with Mikael Boden (SCMB), we are also investigating how changes to chromatin landscapes mediate NSC differentiation, and developing bioinformatic tools to enhance the analysis of RNA-seq and ChIP-seq datasets. Collectively, this work will provide fundamental insights into neural development, as well as insights into human neurodevelopmental disorders that arise as a result of abnormal neural stem cell biology in utero.

Research impacts

The human brain is an incredibly complex organ, consisting of over 100 billion neurons, and even more glial cells. Further adding to this complexity is the fact that there are a wide variety of distinct neuronal subpopulations within the brain, each with different morphological characteristics, neurochemical properties and patterns of connectivity. Amazingly, nearly all of the cells within the brain are derived from a relatively small population of neural stem cells (NSCs) that proliferate, then differentiate, during embryogenesis. Understanding how NSC biology is coordinated, both spatially and temporally, to generate the mature brain remains one of the great challenges in biology. My vision is to reveal the mechanisms that control NSC differentiation within the developing brain, and to apply this knowledge to understand diseases caused by abnormal NSC differentiation, such as autism and hydrocephalus.

I have made a number of significant contributions to understanding how NSC differentiation is coordinated during neural development since starting my own group in late 2010. This work, which was supported by competitive fellowship (NHMRC Career Development Fellowship 2009-2012; ARC Future Fellowship 2013-2017) and grant funding (three NHMRC project grants as CIA; two ARC Discovery Projects as sole CI), has helped to elucidate the fundamental mechanisms underpinning neurogenesis within the neocortex, hippocampus and cerebellum. I have also defined critical molecular controllers of NSC quiescence, a cellular state that ensures the longevity of adult NSCs, as well as describing the behavioural consequences of aberrant adult neurogenesis. Finally, I have provided new insights into how abnormal stem cell biology can contribute to a range of neurodevelopmental disorders, as well as cancers of the brain and skin. The significance of my findings has been recognised by multiple awards for research excellence, from both national (e.g. 2018 Emerging Leader Award, Australian and New Zealand Society for Cell and Developmental Biology; 2010 AW Campbell Award, Australasian Neuroscience Society) and international agencies (2015 Innovator Award, Hydrocephalus Association; 2010 CJ Herrick Award, American Association for Anatomists). I now am in an ideal position to address aspects of two key questions in the field, namely, what are the transcriptomic and epigenomic factors that control the differentiation of NSCs during brain development, and how do deficits in this process contribute to disease?

I have published 111 manuscripts, over 70% of which have been as first or last author. These include manuscripts in leading jourals such as Nature, Nature Neuroscience, Neuron, The Journal of Neuroscience and Cerebral Cortex. For my full publication record, please visit my Orcid site

Search Professor Michael Piper’s works on UQ eSpace

130 works between 2000 and 2025
All (130) Journal Article (116) Book Chapter (5) Conference Publication (8) Other Outputs (1)

21 - 40 of 130 works

2023

Conference Publication

Polycomb Protein EED Regulates Identity Of Glutamatergic Neurons

Currey, Laura, Mitchell, Benjamin, Harris, Lachlan, Thor, Stefan and Piper, Michael (2023). Polycomb Protein EED Regulates Identity Of Glutamatergic Neurons. IBRO 11th World Congress of Neuroscience, Granada, Spain, 9-13 September 2023. Amsterdam, Netherlands: Elsevier. doi: 10.1016/j.ibneur.2023.08.045

Polycomb Protein EED Regulates Identity Of Glutamatergic Neurons

2023

Journal Article

Cytocipher determines significantly different populations of cells in single cell RNA-seq data

Balderson, Brad, Piper, Michael, Thor, Stefan and Boden, Mikael (2023). Cytocipher determines significantly different populations of cells in single cell RNA-seq data. Bioinformatics, 39 (7) btad435. doi: 10.1093/bioinformatics/btad435

Cytocipher determines significantly different populations of cells in single cell RNA-seq data

2023

Journal Article

A mouse model with a frameshift mutation in the nuclear factor I/X (NFIX) gene has phenotypic features of Marshall‐Smith Syndrome

Kooblall, Kreepa G., Stevenson, Mark, Stewart, Michelle, Harris, Lachlan, Zalucki, Oressia, Dewhurst, Hannah, Butterfield, Natalie, Leng, Houfu, Hough, Tertius A., Ma, Da, Siow, Bernard, Potter, Paul, Cox, Roger D., Brown, Stephen D. M., Horwood, Nicole, Wright, Benjamin, Lockstone, Helen, Buck, David, Vincent, Tonia L., Hannan, Fadil M., Bassett, J.H. Duncan, Williams, Graham R., Lines, Kate E., Piper, Michael, Wells, Sara, Teboul, Lydia, Hennekam, Raoul C. and Thakker, Rajesh V. (2023). A mouse model with a frameshift mutation in the nuclear factor I/X (NFIX) gene has phenotypic features of Marshall‐Smith Syndrome. JBMR Plus, 7 (6) e10739, 1-14. doi: 10.1002/jbm4.10739

A mouse model with a frameshift mutation in the nuclear factor I/X (NFIX) gene has phenotypic features of Marshall‐Smith Syndrome

2022

Journal Article

Hydrocephalus in Nfix−/− mice is underpinned by changes in ependymal cell physiology

Harkins, Danyon, Harvey, Tracey J., Atterton, Cooper, Miller, Ingrid, Currey, Laura, Oishi, Sabrina, Kasherman, Maria, Davila, Raul Ayala, Harris, Lucy, Green, Kathryn, Piper, Hannah, Parton, Robert G., Thor, Stefan, Cooper, Helen M. and Piper, Michael (2022). Hydrocephalus in Nfix−/− mice is underpinned by changes in ependymal cell physiology. Cells, 11 (15) 2377, 1-27. doi: 10.3390/cells11152377

Hydrocephalus in Nfix−/− mice is underpinned by changes in ependymal cell physiology

2022

Journal Article

Reciprocal regulation of BRN2 and NOTCH1/2 signaling synergistically drives melanoma cell migration and invasion

Fane, Mitchell E., Chhabra, Yash, Spoerri, Loredana, Simmons, Jacinta L., Ludwig, Raquelle, Bonvin, Elise, Goding, Colin R., Sturm, Richard A., Boyle, Glen M., Haass, Nikolas K., Piper, Michael and Smith, Aaron G. (2022). Reciprocal regulation of BRN2 and NOTCH1/2 signaling synergistically drives melanoma cell migration and invasion. Journal of Investigative Dermatology, 142 (7), 1845-1857. doi: 10.1016/j.jid.2020.12.039

Reciprocal regulation of BRN2 and NOTCH1/2 signaling synergistically drives melanoma cell migration and invasion

2022

Journal Article

Functional divergence of the two Elongator subcomplexes during neurodevelopment

Gaik, Monika, Kojic, Marija, Stegeman, Megan R., Öncü‐Öner, Tülay, Kościelniak, Anna, Jones, Alun, Mohamed, Ahmed, Chau, Pak Yan Stefanie, Sharmin, Sazia, Chramiec‐Głąbik, Andrzej, Indyka, Paulina, Rawski, Michał, Biela, Anna, Dobosz, Dominika, Millar, Amanda, Chau, Vann, Ünalp, Aycan, Piper, Michael, Bellingham, Mark C., Eichler, Evan E., Nickerson, Deborah A., Güleryüz, Handan, Abbassi, Nour El Hana, Jazgar, Konrad, Davis, Melissa J., Mercimek‐Andrews, Saadet, Cingöz, Sultan, Wainwright, Brandon J. and Glatt, Sebastian (2022). Functional divergence of the two Elongator subcomplexes during neurodevelopment. EMBO Molecular Medicine, 14 (7) e15608, e15608. doi: 10.15252/emmm.202115608

Functional divergence of the two Elongator subcomplexes during neurodevelopment

2022

Journal Article

The DUB club: deubiquitinating enzymes and neurodevelopmental disorders

Jolly, Lachlan A., Kumar, Raman, Penzes, Peter, Piper, Michael and Gecz, Jozef (2022). The DUB club: deubiquitinating enzymes and neurodevelopmental disorders. Biological Psychiatry, 92 (8), 614-625. doi: 10.1016/j.biopsych.2022.03.022

The DUB club: deubiquitinating enzymes and neurodevelopmental disorders

2022

Journal Article

Selective requirement for polycomb repressor complex 2 in the generation of specific hypothalamic neuronal subtypes

Yaghmaeian Salmani, Behzad, Balderson, Brad, Bauer, Susanne, Ekman, Helen, Starkenberg, Annika, Perlmann, Thomas, Piper, Michael, Bodén, Mikael and Thor, Stefan (2022). Selective requirement for polycomb repressor complex 2 in the generation of specific hypothalamic neuronal subtypes. Development, 149 (5) dev200076. doi: 10.1242/dev.200076

Selective requirement for polycomb repressor complex 2 in the generation of specific hypothalamic neuronal subtypes

2022

Journal Article

Deletion of NFIX results in defective progression through meiosis within the mouse testis

Davila, Raul Ayala, Spiller, Cassy, Harkins, Danyon, Harvey, Tracey, Jordan, Philip W., Gronostajski, Richard M., Piper, Michael and Bowles, Josephine (2022). Deletion of NFIX results in defective progression through meiosis within the mouse testis. Biology of Reproduction, 106 (6), 1191-1205. doi: 10.1093/biolre/ioac049

Deletion of NFIX results in defective progression through meiosis within the mouse testis

2022

Journal Article

Identifying gene expression profiles associated with neurogenesis and inflammation in the human subependymal zone from development through aging

Bitar, Mainá, Weissleder, Christin, North, Hayley F., Clearwater, Misaki S., Zalucki, Oressia, Halliday, Glenda M., Webster, Maree J., Piper, Michael, Weickert, Cynthia Shannon and Barry, Guy (2022). Identifying gene expression profiles associated with neurogenesis and inflammation in the human subependymal zone from development through aging. Scientific Reports, 12 (1) 40, 40. doi: 10.1038/s41598-021-03976-4

Identifying gene expression profiles associated with neurogenesis and inflammation in the human subependymal zone from development through aging

2021

Journal Article

Cep55 regulation of PI3K/Akt signaling is required for neocortical development and ciliogenesis

Rashidieh, Behnam, Shohayeb, Belal, Bain, Amanda Louise, Fortuna, Patrick R. J., Sinha, Debottam, Burgess, Andrew, Mills, Richard, Adams, Rachael C., Lopez, J. Alejandro, Blumbergs, Peter, Finnie, John, Kalimutho, Murugan, Piper, Michael, Hudson, James Edward, Ng, Dominic C. H. and Khanna, Kum Kum (2021). Cep55 regulation of PI3K/Akt signaling is required for neocortical development and ciliogenesis. PLoS Genetics, 17 (10) e1009334, 1-31. doi: 10.1371/journal.pgen.1009334

Cep55 regulation of PI3K/Akt signaling is required for neocortical development and ciliogenesis

2021

Journal Article

Genome-wide transcriptomic analysis of the forebrain of postnatal Slc13a4+/− mice

Harvey, Tracey J., Davila, Raul Ayala, Vidovic, Diana, Sharmin, Sazia, Piper, Michael and Simmons, David G. (2021). Genome-wide transcriptomic analysis of the forebrain of postnatal Slc13a4+/− mice. BMC Research Notes, 14 (1) 269, 269. doi: 10.1186/s13104-021-05687-5

Genome-wide transcriptomic analysis of the forebrain of postnatal Slc13a4+/− mice

2021

Journal Article

ChIP-R: Assembling reproducible sets of ChIP-seq and ATAC-seq peaks from multiple replicates

Newell, Rhys, Pienaar, Richard, Balderson, Brad, Piper, Michael, Essebier, Alexandra and Bodén, Mikael (2021). ChIP-R: Assembling reproducible sets of ChIP-seq and ATAC-seq peaks from multiple replicates. Genomics, 113 (4), 1855-1866. doi: 10.1016/j.ygeno.2021.04.026

ChIP-R: Assembling reproducible sets of ChIP-seq and ATAC-seq peaks from multiple replicates

2021

Journal Article

TEAD family transcription factors in development and disease

Currey, Laura, Thor, Stefan and Piper, Michael (2021). TEAD family transcription factors in development and disease. Development, 148 (12) dev196675. doi: 10.1242/dev.196675

TEAD family transcription factors in development and disease

2021

Journal Article

Reduced adult neurogenesis is associated with increased macrophages in the subependymal zone in schizophrenia

Weissleder, Christin, North, Hayley F., Bitar, Maina, Fullerton, Janice M., Sager, Rachel, Barry, Guy, Piper, Michael, Halliday, Glenda M., Webster, Maree J. and Shannon Weickert, Cynthia (2021). Reduced adult neurogenesis is associated with increased macrophages in the subependymal zone in schizophrenia. Molecular Psychiatry, 26 (11), 6880-6895. doi: 10.1038/s41380-021-01149-3

Reduced adult neurogenesis is associated with increased macrophages in the subependymal zone in schizophrenia

2021

Journal Article

Elp2 mutations perturb the epitranscriptome and lead to a complex neurodevelopmental phenotype

Kojic, Marija, Gawda, Tomasz, Gaik, Monika, Begg, Alexander, Salerno-Kochan, Anna, Kurniawan, Nyoman D., Jones, Alun, Drożdżyk, Katarzyna, Kościelniak, Anna, Chramiec-Głąbik, Andrzej, Hediyeh-Zadeh, Soroor, Kasherman, Maria, Shim, Woo Jun, Sinniah, Enakshi, Genovesi, Laura A., Abrahamsen, Rannvá K., Fenger, Christina D., Madsen, Camilla G., Cohen, Julie S., Fatemi, Ali, Stark, Zornitza, Lunke, Sebastian, Lee, Joy, Hansen, Jonas K., Boxill, Martin F., Keren, Boris, Marey, Isabelle, Saenz, Margarita S., Brown, Kathleen ... Wainwright, Brandon J. (2021). Elp2 mutations perturb the epitranscriptome and lead to a complex neurodevelopmental phenotype. Nature Communications, 12 (1) 2678, 2678. doi: 10.1038/s41467-021-22888-5

Elp2 mutations perturb the epitranscriptome and lead to a complex neurodevelopmental phenotype

2021

Journal Article

Perineuronal net abnormalities in Slc13a4+/- mice are rescued by postnatal administration of N-acetylcysteine

Sharmin, Sazia, Pradhan, Jonu, Zhang, Zhe, Bellingham, Mark, Simmons, David and Piper, Michael (2021). Perineuronal net abnormalities in Slc13a4+/- mice are rescued by postnatal administration of N-acetylcysteine. Experimental Neurology, 342 113734, 1-16. doi: 10.1016/j.expneurol.2021.113734

Perineuronal net abnormalities in Slc13a4+/- mice are rescued by postnatal administration of N-acetylcysteine

2021

Journal Article

Editorial: Context-dependent regulation of neurogenesis: common themes and unique features of the neurogenic process in different model systems

Lupo, Giuseppe, Piper, Michael and Zolessi, Flavio R. (2021). Editorial: Context-dependent regulation of neurogenesis: common themes and unique features of the neurogenic process in different model systems. Frontiers in Cell and Developmental Biology, 9 678475, 678475. doi: 10.3389/fcell.2021.678475

Editorial: Context-dependent regulation of neurogenesis: common themes and unique features of the neurogenic process in different model systems

2020

Journal Article

Conserved epigenetic regulatory logic infers genes governing cell identity

Shim, Woo Jun, Sinniah, Enakshi, Xu, Jun, Vitrinel, Burcu, Alexanian, Michael, Andreoletti, Gaia, Shen, Sophie, Sun, Yuliangzi, Balderson, Brad, Boix, Carles, Peng, Guangdun, Jing, Naihe, Wang, Yuliang, Kellis, Manolis, Tam, Patrick P L, Smith, Aaron, Piper, Michael, Christiaen, Lionel, Nguyen, Quan, Bodén, Mikael and Palpant, Nathan J. (2020). Conserved epigenetic regulatory logic infers genes governing cell identity. Cell Systems, 11 (6), 625-639.e13. doi: 10.1016/j.cels.2020.11.001

Conserved epigenetic regulatory logic infers genes governing cell identity

2020

Journal Article

Missense variant contribution to USP9X-female syndrome

Jolly, Lachlan A., Parnell, Euan, Gardner, Alison E., Corbett, Mark A., Pérez-Jurado, Luis A., Shaw, Marie, Lesca, Gaetan, Keegan, Catherine, Schneider, Michael C., Griffin, Emily, Maier, Felicitas, Kiss, Courtney, Guerin, Andrea, Crosby, Kathleen, Rosenbaum, Kenneth, Tanpaiboon, Pranoot, Whalen, Sandra, Keren, Boris, McCarrier, Julie, Basel, Donald, Sadedin, Simon, White, Susan M., Delatycki, Martin B., Kleefstra, Tjitske, Küry, Sébastien, Brusco, Alfredo, Sukarova-Angelovska, Elena, Trajkova, Slavica, Yoon, Sehoun ... Gecz, Jozef (2020). Missense variant contribution to USP9X-female syndrome. npj Genomic Medicine, 5 (1) 53, 1-11. doi: 10.1038/s41525-020-00162-9

Missense variant contribution to USP9X-female syndrome

Current funding

  • 2023 - 2026
    What drives the Anterior Expansion of the Central Nervous System?
    ARC Discovery Projects
    Open grant
  • 2023 - 2025
    What is the common factor driving brain overgrowth in ASD? Investigating the relationship between epigenetic marks neural stem cell proliferation.
    Simons Foundation Autism Research Initiative - Pilot Award
    Open grant

Past funding

  • 2023 - 2024
    Generation and characterisation of humanised mouse model of Malan Syndrome
    The University of Queensland in America, Inc
    Open grant
  • 2023 - 2024
    The Brain-Ovary connection: identification of a novel regulator of female reproductive function
    Repro Grants
    Open grant
  • 2022 - 2025
    Understanding the generation of hypothalamic sleep neurons
    ARC Discovery Projects
    Open grant
  • 2021 - 2023
    Can inhalational general anaesthetic exposure during pregnancy affect non-genetic heritable elements in fetal germs cells in such a way as to engender pathology in offspring,
    Silicon Valley Community Foundation
    Open grant
  • 2019
    Advanced Brightfield and Fluorescent High Speed and Throughput Slide Scanner for biological, medical, materials science, and agricultural applications
    UQ Major Equipment and Infrastructure
    Open grant
  • 2018
    Trailblazer Grant Piper ISDN Meeting 2018
    Brisbane Marketing
    Open grant
  • 2018 - 2021
    Transcriptional regulation of brain size during development
    ARC Discovery Projects
    Open grant
  • 2018 - 2020
    Aberrant ependymal development and the formation of hydrocephalus
    NHMRC Project Grant
    Open grant
  • 2017 - 2019
    USP9X: A master gene for neural development and autism
    Simons Foundation Autism Research Initiative
    Open grant
  • 2016 - 2019
    Molecular control of adult neural stem cell quiescence
    ARC Discovery Projects
    Open grant
  • 2016 - 2017
    Regulation of stem cell differentiation during cerebellar development and medulloblastoma
    Cancer Council Queensland
    Open grant
  • 2015 - 2016
    Analysis of the role of NFIX in the development of hydrocephalus
    Hydrocephalus Association Innovator Award Research Grant
    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
    Mitochondrial analysis suite
    UQ Major Equipment and Infrastructure
    Open grant
  • 2014 - 2016
    Regulation of neural progenitor cell self-renewal by the RNA-binding protein ZFP36L1 during development and disease
    NHMRC Project Grant
    Open grant
  • 2014
    Touchscreen-automated cognitive testing for mice
    NHMRC Equipment Grant
    Open grant
  • 2013 - 2017
    Transcriptional control of neural stem cell differentiation during development and disease
    ARC Future Fellowships
    Open grant
  • 2013
    Establishment of an Integrated Facility for Single Cell Analysis
    UQ Major Equipment and Infrastructure
    Open grant
  • 2012 - 2014
    Nfib regulates glial differentiation during development and disease via repression of the key epigenetic protein, Ezh2
    NHMRC Project Grant
    Open grant
  • 2011 - 2013
    Investigation of the role of Nfix in adult neurogenesis
    NHMRC Project Grant
    Open grant
  • 2011 - 2013
    ResTeach 2011 0.1 FTE School of Biomedical Sciences
    UQ ResTeach
    Open grant
  • 2011 - 2012
    Suppression of high-grade glioma by Nfib overexpression
    Cancer Council Queensland
    Open grant
  • 2010 - 2012
    Regulation of the Polycomb Genes Eed and Ezh2 by Nfib during Neural Progenitor Cell Differentiation
    UQ Foundation Research Excellence Awards - DVC(R) Funding
    Open grant
  • 2010
    The role of Nfix in stem cell differentiation within the subventricular zone of the adult brain
    UQ Early Career Researcher
    Open grant
  • 2009 - 2013
    NHMRC Career Development Award (Biomedical Level 1): Nfi genes regulate the switch between neurogenesis and gliogenesis during cortical development
    NHMRC Career Development Award
    Open grant
  • 2007 - 2008
    Analysis of gene expression changes within the cortex of Nfi- and Emx1-deficient mice
    UQ New Staff Research Start-Up Fund
    Open grant
  • 2007 - 2008
    The role of Nfi genes in development of the corpus callosum
    Ramaciotti Foundation
    Open grant

Availability

Professor Michael Piper is:
Available for supervision

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Available projects

  • Understanding the drivers of neural stem cell differentiation

    What are the mechanisms that control neural stem cell (NSC) differentiation during embryogenesis, and that enable the generation of the diverse suite of neurons and glia that comprise the brain? This is a key question in developmental neuroscience. My contribution to this field to date has been to reveal central transcriptional regulators that mediate NSC biology within the brain. Using rodent model systems, I demonstrated that transcription factors of the Nuclear Factor One (NFI) family mediate NSC proliferation and differentiation in the embryonic, postnatal and adult nervous system. This work has received international recognition, as evidenced by numerous invited international presentations and high-impact reviews (e.g. Trends in Cell Biology), and forms the framework around which the hypotheses of this program will be addressed.

    I am interested in defining how NSC proliferation and differentiation is regulated at a transcriptional and epigenomic level within the developing nervous system. Using the developing mouse brain as a model system, we are using a suite of molecular and cellular techniques to understand how diverse regions of the nervous system are generated, including the cerebral cortex, the cerebellum, the spinal cord and the hypothalamus. For example, within the cerebral cortex, we are investigating how the NFI family of transcription factors mediate NSC differentiation, and how mutations to the NFI family culminate in macrocephaly, and disorders such as Malan syndrome. Moreover, we are using mice lacking the gene Nsd1(a histone modifying protein) to investigate the development of a human syndrome known as Sotos syndrome, which is also characterised by macrocephaly. In collaboration with Mikael Boden (SCMB), we are also investigating how changes to chromatin landscapes mediate NSC differentiation, and developing bioinformatic tools to enhance the analysis of RNA-seq and ChIP-seq datasets. Collectively, this work will provide fundamental insights into neural development, as well as insights into human neurodevelopmental disorders that arise as a result of abnormal neural stem cell biology in utero.

  • Adult neurogenesis

    The birth of new neurons within the mature cerebral cortex, a process termed neurogenesis, plays a critical role in learning, memory and spatial navigation. We are investigating various aspects of adult neurogenesis in rodent models, such as neural stem cell quiescence . We are also interrogating the consequences of abnormal neurogenesis using behavioural tests for learning and memory.

    We employ a range of transgenic mice to investigate adult neurogenesis, coupled with techniques ranging from immunocytochemistry, behavioural testing, analysis of axonal connectivity and genome-wide sequencing platforms. Given the critical roles that learning and memory play in our everyday lives, and the fact that neurogenesis within the adult brain diminishes with age, this research will provide fundamental insights into how this vital process is co-ordinated at a cellular and molecular level.

  • Identifying how abnormal neural stem cell biology contributes to disease

    The importance of NSC biology to brain development is underscored by disorders associated with abnormal NSC differentiation, including autism, hydrocephalus and macrocephaly. Despite the role of aberrant NSC development to these disorders, our understanding of the cellular and molecular deficits that contribute to disease onset and progression remains limited. Recently, my work has begun to focus on these disorders. Moreover, as the transcriptional landscape of many cancers resembles that of stem cells during development, I am also applying my expertise to understand how abnormal transcriptional activity contributes to cancer progression. This approach has gained significant traction, as evidenced by international awards (2015 Innovator Award, Hydrocephalus Association) and grants (Simons Foundation Autism Research Initiative, 2018-2019; Cancer Council Queensland, 2016-2017) I have received.

  • Understanding the drivers of neural stem cell differentiation

    What are the mechanisms that control neural stem cell (NSC) differentiation during embryogenesis, and that enable the generation of the diverse suite of neurons and glia that comprise the brain? This is a key question in developmental neuroscience. My contribution to this field to date has been to reveal central transcriptional regulators that mediate NSC biology within the brain. Using rodent model systems, I demonstrated that transcription factors of the Nuclear Factor One (NFI) family mediate NSC proliferation and differentiation in the embryonic, postnatal and adult nervous system. This work has received international recognition, as evidenced by numerous invited international presentations and high-impact reviews (e.g. Trends in Cell Biology), and forms the framework around which the hypotheses of this program will be addressed.

    I am interested in defining how NSC proliferation and differentiation is regulated at a transcriptional and epigenomic level within the developing nervous system. Using the developing mouse brain as a model system, we are using a suite of molecular and cellular techniques to understand how diverse regions of the nervous system are generated, including the cerebral cortex, the cerebellum, the spinal cord and the hypothalamus. For example, within the cerebral cortex, we are investigating how the NFI family of transcription factors mediate NSC differentiation, and how mutations to the NFI family culminate in macrocephaly, and disorders such as Malan syndrome. Moreover, we are using mice lacking the gene Nsd1(a histone modifying protein) to investigate the development of a human syndrome known as Sotos syndrome, which is also characterised by macrocephaly. In collaboration with Mikael Boden (SCMB), we are also investigating how changes to chromatin landscapes mediate NSC differentiation, and developing bioinformatic tools to enhance the analysis of RNA-seq and ChIP-seq datasets. Collectively, this work will provide fundamental insights into neural development, as well as insights into human neurodevelopmental disorders that arise as a result of abnormal neural stem cell biology in utero.

  • Adult neurogenesis

    The birth of new neurons within the mature cerebral cortex, a process termed neurogenesis, plays a critical role in learning, memory and spatial navigation. We are investigating various aspects of adult neurogenesis in rodent models, such as neural stem cell quiescence . We are also interrogating the consequences of abnormal neurogenesis using behavioural tests for learning and memory.

    We employ a range of transgenic mice to investigate adult neurogenesis, coupled with techniques ranging from immunocytochemistry, behavioural testing, analysis of axonal connectivity and genome-wide sequencing platforms. Given the critical roles that learning and memory play in our everyday lives, and the fact that neurogenesis within the adult brain diminishes with age, this research will provide fundamental insights into how this vital process is co-ordinated at a cellular and molecular level.

  • Identifying how abnormal neural stem cell biology contributes to disease

    The importance of NSC biology to brain development is underscored by disorders associated with abnormal NSC differentiation, including autism, hydrocephalus and macrocephaly. Despite the role of aberrant NSC development to these disorders, our understanding of the cellular and molecular deficits that contribute to disease onset and progression remains limited. Recently, my work has begun to focus on these disorders. Moreover, as the transcriptional landscape of many cancers resembles that of stem cells during development, I am also applying my expertise to understand how abnormal transcriptional activity contributes to cancer progression. This approach has gained significant traction, as evidenced by international awards (2015 Innovator Award, Hydrocephalus Association) and grants (Simons Foundation Autism Research Initiative, 2018-2019; Cancer Council Queensland, 2016-2017) I have received.

Supervision history

Current supervision

Completed supervision

Enquiries

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