Professor Kate Schroder
Professor

Kate Schroder

Email: 
Phone: 
+61 7 334 62058

Background

Professor Kate Schroder heads the Inflammasome Laboratory and is Director of the Centre for Inflammation and Disease Research at the Institute for Molecular Bioscience (IMB), University of Queensland, as an NHMRC Leadership Fellow. Kate’s graduate studies defined novel macrophage activation mechanisms and her subsequent postdoctoral research identified surprising inter-species divergence in the inflammatory programs of human versus mouse macrophages. As an NHMRC CJ Martin Fellow in Switzerland, Kate trained with the pioneer of inflammasome biology, Jürg Tschopp. The IMB Inflammasome Laboratory, which Kate heads, investigates the molecular mechanisms governing inflammasome activity and caspase activation, the cellular mediators of inflammasome-dependent inflammation, and mechanisms of inflammasome inhibition by cellular pathways and small molecule inhibitors.

Kate is a co-inventor on patents for small molecule inhibitors of the NLRP3 inflammasome, currently under commercialisation by Inflazome Ltd. Inflazome Ltd was recently acquired by Roche in a landmark deal – one of the largest in Australian and Irish biotech history. The acquisition gives Roche full rights to Inflazome’s portfolio of inflammasome inhibitors. Two of the company’s drug candidates are in clinical trials for the treatment of debilitating conditions such as cardiovascular disease, arthritis and neurodegenerative diseases such as Parkinson’s, Alzheimer’s and motor neuron disease.

Kate has authored more than 140 publications, featuring in journals such as Science, Cell, Nature Genetics, Nature Medicine, Nature Chemical Biology, Journal of Experimental Medicine and PNAS USA, and her work has been cited more than 35,000 times. Kate is an Editorial Board Member for international journals including Science Signaling, Clinical and Translational Immunology and Cell Death Disease. She is the recipient of the 2022 Women in Technology Excellence in Science Award, 2020 Nancy Mills Award for Women in Science, 2019 ANZSCDB Emerging Leader Award, 2019 Merck Research Medal, 2014 Milstein Young Investigator Award, 2013 Tall Poppy Award, 2012 Gordon Ada Career Award, 2010 QLD Premier’s Postdoctoral Award, and the 2008 Society for Leukocyte Biology’s Dolph Adams Award.

INFLAMMASOME LABORATORY RESEARCH

During injury or infection, our body’s immune system protects us by launching inflammation. But uncontrolled inflammation drives diseases such as gout, diabetes, neurodegenerative disease and cancer. The Inflammasome Lab is defining the molecular and cellular processes of inflammation. We seek to unravel the secrets of inflammasomes – protein complexes at the heart of inflammation and disease – to allow for new therapies to fight human diseases.

The Inflammasome Laboratory integrates molecular and cell biology approaches with in vivo studies to gain a holistic understanding of inflammasome function during infection, and inflammasome dysfunction in human inflammatory disease. Current research interests include the molecular mechanisms governing inflammasome activity and caspase activation, the cellular mediators of inflammasome-dependent inflammation, and inflammasome suppression by autophagy and small molecule inhibitors.

Availability

Professor Kate Schroder is:
Available for supervision
Media expert

Fields of research

Biological Sciences Genetics Immunology

Qualifications

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

Research impacts

Our research focuses on understanding how immune cells launch healthy inflammation to fight infection and unhealthy inflammation to promote disease. By understanding exactly how the body fights infection, we can help identify new drug targets or vaccines to combat infectious disease, which causes 13 million deaths globally each year. By understanding how unhealthy inflammation is initiated, we may also be able to design new strategies for the treatment of common diseases such as cancer, gout and diabetes.

Search Professor Kate Schroder’s works on UQ eSpace

174 works between 2001 and 2025
All (174) Journal Article (148) Book Chapter (7) Conference Publication (14) Other Outputs (5)

161 - 174 of 174 works

2008

Conference Publication

Primary murine osteoblast cultures contain macrophages that enhance osteoblast mineralisation

Chang, M. K., Pettit, A. R., Schroder, K., Ripoll, V. M., Alexander, K. A., Hume, D. A. and Raggatt, L. (2008). Primary murine osteoblast cultures contain macrophages that enhance osteoblast mineralisation. ECTS 35th European Symposium on Calcified Tissues, Barcelona, Spain, 24-28 May 2008. New York, NY, U.S.A.: Springer New York. doi: 10.1007/s00223-008-9118-5

Primary murine osteoblast cultures contain macrophages that enhance osteoblast mineralisation

2007

Journal Article

Differential effects of CpG DNA on IFN-beta induction and STAT1 activation in murine macrophages versus dendritic cells: Alternatively activated STAT1 negatively regulates TLR signaling in macrophages

Schroder, K., Spille, M., Pilz, A., Lattin, J., Bode, K. A., Irvine, K. M., Burrows, A. D., Ravasi, T., Weighardt, H., Stacey, K. J., Decker, T., Hume, D. A., Dalpke, A. H. and Sweet, M. J. (2007). Differential effects of CpG DNA on IFN-beta induction and STAT1 activation in murine macrophages versus dendritic cells: Alternatively activated STAT1 negatively regulates TLR signaling in macrophages. Journal of Immunology, 179 (6), 3495-3503. doi: 10.4049/jimmunol.179.6.3495

Differential effects of CpG DNA on IFN-beta induction and STAT1 activation in murine macrophages versus dendritic cells: Alternatively activated STAT1 negatively regulates TLR signaling in macrophages

2007

Journal Article

G-protein-coupled receptor expression, function, and signaling in macrophages

Lattin, J., Zidar, D., Schroder, K., Kellie, S., Hume, D. and Sweet, M. (2007). G-protein-coupled receptor expression, function, and signaling in macrophages. Journal of Leukocyte Biology, 82 (1), 16-32. doi: 10.1189/jlb.0107051

G-protein-coupled receptor expression, function, and signaling in macrophages

2007

Journal Article

PU.1 and ICSBP control constitutive and IFN-gamma-regulated Tlr9 gene expression in mouse macrophages

Schroder, Kate, Lichtinger, Monika, Irvine, Katharine M., Brion, Kristian, Trieu, Angela, Ross, Ian L., Ravasi, Timothy, Stacey, Katryn J., Rehli, Michael, Hume, David A. and Sweet, Matthew J. (2007). PU.1 and ICSBP control constitutive and IFN-gamma-regulated Tlr9 gene expression in mouse macrophages. Journal of Leukocyte Biology, 81 (6), 1577-1590. doi: 10.1189/jlb.0107036

PU.1 and ICSBP control constitutive and IFN-gamma-regulated Tlr9 gene expression in mouse macrophages

2007

Conference Publication

Primary Murine Osteoblast Cultures Contain Macrophages that Enhance Osteoblast Mineralisation

Chang, M., Hume, D. A., Pettit, A. R., Raggatt, L., Ripoll, V. M. and Schroder, K. (2007). Primary Murine Osteoblast Cultures Contain Macrophages that Enhance Osteoblast Mineralisation. 29th Annual Meeting of the American Society for Bone and Mineral Research (ASBMR), Honolulu, Hawaii, USA, 16th - 19th September, 2007. Washington, D. C.: American Society for Bone and Mineral Research.

Primary Murine Osteoblast Cultures Contain Macrophages that Enhance Osteoblast Mineralisation

2007

Journal Article

Histone deacetylase inhibitors decrease Toll-like receptor-mediated activation of proinflammatory gene expression by impairing transcription factor recruitment

Bode, K. A., Schroder, K., Hume, D. A., Ravasi, T., Heeg, K., Sweet, M. J. and Dalpke, A. H. (2007). Histone deacetylase inhibitors decrease Toll-like receptor-mediated activation of proinflammatory gene expression by impairing transcription factor recruitment. Immunology, 122 (4), 596-606. doi: 10.1111/j.1365-2567.2007.02678.x

Histone deacetylase inhibitors decrease Toll-like receptor-mediated activation of proinflammatory gene expression by impairing transcription factor recruitment

2006

Journal Article

Alternate transcription of the Toll-like receptor signaling cascade

Wells, C. A., Chalk, A. M., Forrest, A., Taylor, D., Waddell, N., Schroder, K., Himes, S. R., Faulkner, G., Lo, S., Kasukawa, T., Kawaji, H., Kai, C., Kawai, J., Katayama, S., Carninci, P., Hayashizaki, Y., Hume, D. A. and Grimmond, S. M. (2006). Alternate transcription of the Toll-like receptor signaling cascade. Genome Biology, 7 (2) R10, R10.1-R10.17. doi: 10.1186/gb-2006-7-2-r10

Alternate transcription of the Toll-like receptor signaling cascade

2006

Journal Article

LPS regulates proinflammatory gene expression in macrophages by altering histone deacetylase expression

Aung, H. T., Schroder, K., Himes, S. R., Brion, K., van Zuylen, W., Trieu, A., Suzuki, H., Hayashizaki, Y., Hume, D. A., Sweet, M. J. and Ravasi, T. (2006). LPS regulates proinflammatory gene expression in macrophages by altering histone deacetylase expression. Faseb Journal, 20 (9), 1315-1327. doi: 10.1096/fj.05-5360com

LPS regulates proinflammatory gene expression in macrophages by altering histone deacetylase expression

2006

Journal Article

Signal integration between IFN gamma and TLR signalling pathways in macrophages

Schroder, K., Sweet, M. J. and Hume, D. A. (2006). Signal integration between IFN gamma and TLR signalling pathways in macrophages. Immunobiology, 211 (6-8), 511-524. doi: 10.1016/j.imbio.2006.05.007

Signal integration between IFN gamma and TLR signalling pathways in macrophages

2005

Conference Publication

PU.1 and ICSBP regulate the tlr9 promoter in mouse macrophages

Schroder, Kate, Irvine, Katharine M., Biron, Kristian, Lichtinger, Monika, Ravasi, Timothy, Rehli, Michael, Sweet, Matthen J. and Hume, David A. (2005). PU.1 and ICSBP regulate the tlr9 promoter in mouse macrophages. BASEL: BIRKHAUSER VERLAG AG.

PU.1 and ICSBP regulate the tlr9 promoter in mouse macrophages

2005

Other Outputs

Mechanisms of IFN[gamma] priming of macrophage activation by CpG DNA

Schroder, Kate (2005). Mechanisms of IFN[gamma] priming of macrophage activation by CpG DNA. PhD Thesis, Institute for Molecular Bioscience, The University of Queensland. doi: 10.14264/295470

Mechanisms of IFN[gamma] priming of macrophage activation by CpG DNA

2005

Journal Article

LPS regulates a set of genes in primary murine macrophages by antagonising CSF-1 action

Sester, D. P., Trieu, A., Brion, K., Schroder, K., Ravasi, T., Robinson, J. A., McDonald, R. C., Ripoll, V., Wells, C. A., Suzuki, H., Hayashizaki, Y., Stacey, K. J., Hume, D. A. and Sweet, M. J. (2005). LPS regulates a set of genes in primary murine macrophages by antagonising CSF-1 action. Immunobiology, 210 (2-4), 97-107. doi: 10.1016/j.imbio.2005.05.004

LPS regulates a set of genes in primary murine macrophages by antagonising CSF-1 action

2004

Journal Article

Probing the S100 protein family through genomic and functional analysis

Ravasi, Timothy, Hsu, Kenneth, Goyette, Jesse, Schroder, Kate, Yang, Zheng, Rahimi, Farid, Miranda, Les P., Alewood, Paul F., Hume, David A. and Geczy, Carolyn (2004). Probing the S100 protein family through genomic and functional analysis. Genomics, 84 (1), 10-22. doi: 10.1016/j.ygeno.2004.02.002

Probing the S100 protein family through genomic and functional analysis

2001

Journal Article

Activity of recombinant dengue 2 virus NS3 protease in the presence of a truncated NS2B co-factor, small peptide substrates, and inhibitors

Leung, D., Schroder, K., White, H., Fang, N. X., Stoermer, M. J., Abbenante, G., Martin, J. L., Young, P. R. and Fairlie, D. P. (2001). Activity of recombinant dengue 2 virus NS3 protease in the presence of a truncated NS2B co-factor, small peptide substrates, and inhibitors. Journal of Biological Chemistry, 276 (49), 45762-45771. doi: 10.1074/jbc.M107360200

Activity of recombinant dengue 2 virus NS3 protease in the presence of a truncated NS2B co-factor, small peptide substrates, and inhibitors

Current funding

  • 2025 - 2027
    A novel signalling effector of ASC pyroptosomes
    ARC Discovery Projects
    Open grant
  • 2024 - 2025
    Hope on the horizon - Harnessing inflammation as a novel diagnostic for chronic liver disease (2024 MSHRSS Co-funded Collaboration Grant led by MSH)
    Metro South Health Research Support Scheme Project Grant
    Open grant
  • 2023 - 2026
    Pyroptotic macrophages posthumously sculpt immune responses
    ARC Discovery Projects
    Open grant
  • 2022 - 2026
    Inflammasome inhibitors as new first-in-class anti-inflammatory therapies
    NHMRC Investigator Grants
    Open grant
  • 2022 - 2026
    Mining the host-pathogen interface to deliver a drug pipeline for treating intractable and emerging infections
    NHMRC Synergy Grants
    Open grant

Past funding

  • 2023 - 2024
    Elucidating Cardiolipin and Immune Dysfunction in Barth Syndrome
    The Barth Syndrome Foundation
    Open grant
  • 2022 - 2025
    Nuclear alarmins escalate tissue immune responses
    ARC Discovery Projects
    Open grant
  • 2021 - 2023
    Accelerating the diagnosis of children with autoinflammatory diseases
    Specific Donations Research Grant
    Open grant
  • 2020 - 2022
    A novel mechanism of host defence via macrophage extracellular traps
    ARC Discovery Projects
    Open grant
  • 2019 - 2021
    Developing treatments for vincristine-induced neuropathy
    The Kid's Cancer Project
    Open grant
  • 2019 - 2023
    Pathogenic functions for the NLRP3 inflammasome in Alzheimer's Disease
    The Yulgilbar Foundation
    Open grant
  • 2019 - 2022
    Molecular determinants of inflammatory caspase activity upon inflammasomes
    ARC Discovery Projects
    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
  • 2019
    In vivo imaging system for tracking inflammation, infection, cancer, pain and bioactive molecules
    UQ Major Equipment and Infrastructure
    Open grant
  • 2019 - 2021
    PyroNETosis: a new mechanism of host defence
    NHMRC Project Grant
    Open grant
  • 2018
    Epifluorescent and live-cell imaging microscopes for the investigation of host-pathogen interactions and for molecular and cellular biology
    UQ Major Equipment and Infrastructure
    Open grant
  • 2018 - 2021
    Extinguishing the fire: inflammasome inhibition
    NHMRC Career Development Fellowship
    Open grant
  • 2017 - 2024
    ACRF Cancer Ultrastructure and Function Facility
    Australian Cancer Research Foundation
    Open grant
  • 2017 - 2019
    A novel mechanism for IL-1B secretion
    NHMRC Project Grant
    Open grant
  • 2017 - 2019
    Inflammatory pathways to liver fibrosis in non-alcoholic and alcoholic steatohepatitis: reversal by NLRP3 inhibitors (NHMRC Project Grant administered by ANU)
    Australian National University
    Open grant
  • 2016 - 2018
    Pharmacological Targeting of Proinflammatory Kinase Signalling in Parkinson's disease
    The Michael J Fox Foundation for Parkinsons Research
    Open grant
  • 2016 - 2020
    Blocking inflammasome-induced neuroinflammation in PD with a potent, orally available small molecule
    The Michael J Fox Foundation Therapeutic Pipeline Program
    Open grant
  • 2016 - 2019
    A molecular timer for inflammation and cell death
    ARC Discovery Projects
    Open grant
  • 2016 - 2018
    Autophagic suppression of ASC inflammasomes
    NHMRC Project Grant
    Open grant
  • 2015 - 2017
    Pharmacological targeting of the NLRP3 inflammasome in pre-clinical models of Parkinson's disease using a potent orally active inhibitor
    The Michael J Fox Foundation for Parkinsons Research
    Open grant
  • 2015 - 2017
    Inhibitors of NLRP3 activation for treatment of inflammatory CNS diseases
    NHMRC Project Grant
    Open grant
  • 2015
    Murine behavioural phenotyping facility
    UQ Major Equipment and Infrastructure
    Open grant
  • 2015 - 2016
    Therapeutic targeting of the NLRP3 inflammasome using a potent and orally active inhibitor in experimental MND
    Motor Neurone Disease Research Institute of Australia Inc
    Open grant
  • 2014 - 2018
    Inflammasomes: molecular drivers of anti-microbial defence
    ARC Future Fellowships
    Open grant
  • 2014 - 2016
    Microbial evasion of a novel inflammasome by Salmonella
    NHMRC Project Grant
    Open grant
  • 2014
    Pinpointing the initiation of immune responses
    UQ Foundation Research Excellence Awards - DVC(R) Funding
    Open grant
  • 2013 - 2016
    Caspase 8 apoptotic signalling induced by the inflammasome
    NHMRC Project Grant
    Open grant
  • 2013 - 2015
    Smart Futures Fellowship (Mid): Development of strategies to predict type 2 diabetes risk, and prevent diabetes onset in at-risk Queensland children
    Queensland Government Smart Futures Fellowships
    Open grant
  • 2012 - 2014
    Inflammasome function in neutrophils
    NHMRC Project Grant
    Open grant
  • 2011 - 2012
    NHMRC Training Fellowship (CJ Martin): Inflammasome function in gastrointestinal immunity and inflammation
    NHMRC Training (Postdoctoral) Fellowship
    Open grant
  • 2005 - 2008
    Human macrophage transcriptional network
    Riken Genomic Sciences Center
    Open grant

Availability

Professor Kate Schroder is:
Available for supervision

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Available projects

  • Student projects

    Expressions of interest from prospective postgraduate students are welcome at any time. For information on future research higher degree projects, please email K.Schroder@imb.uq.edu.au with the following: (1) CV, including a summary of academic qualifications, work and research experience, and publication list; (2) studies report for undergraduate and honours degree(s); and (3) a letter of motivation outlining your research interests.

Supervision history

Current supervision

  • Doctor Philosophy

    Mechanisms of virus-induced NLRP1 Inflammasome Signalling

    Principal Advisor

    Other advisors: Dr Larisa Labzin

  • Doctor Philosophy

    Mechanisms of Inflammasome Assembly and Signalling

    Principal Advisor

  • Doctor Philosophy

    Inflammasome inhibition by molecular and cellular processes in fibrosis (e.g. systemic sclerosis)

    Principal Advisor

    Other advisors: Dr Sabrina Sofia Burgener

  • Doctor Philosophy

    Inflammasomes in tissue homeostasis and wound healing

    Principal Advisor

    Other advisors: Dr Sabrina Sofia Burgener

  • Doctor Philosophy

    Molecular pathways by which human epithelia and macrophages sense and respond to Influenza A virus infection.

    Associate Advisor

    Other advisors: Professor Kirsty Short, Dr Larisa Labzin

  • Doctor Philosophy

    Investigating how antibodies against Influenza A Virus modulate macrophage sensing and signalling pathways and outputs.

    Associate Advisor

    Other advisors: Professor Kirsty Short, Dr Larisa Labzin

  • Doctor Philosophy

    Molecular pathways by which human epithelia and macrophages sense and respond to Influenza A virus infection.

    Associate Advisor

    Other advisors: Professor Kirsty Short, Dr Larisa Labzin

  • Doctor Philosophy

    Discovery and Pharmacological Evaluation of Novel Analgesics for the Relief of Ross River Virus Induced Chronic Pain

    Associate Advisor

    Other advisors: Dr Andy Kuo, Emeritus Professor Maree Smith, Dr Mohammad Zafar Imam

  • Doctor Philosophy

    Inflammasome inhibitors in disease: Is there a therapeutic trade-off of compromised host defence?

    Associate Advisor

    Other advisors: Professor Avril Robertson, Dr Sabrina Sofia Burgener

  • Doctor Philosophy

    Molecular pathways by which human epithelia and macrophages sense and respond to Influenza A virus infection.

    Associate Advisor

    Other advisors: Professor Kirsty Short, Dr Larisa Labzin

  • Doctor Philosophy

    Studying the synergistic effects of streptococcal SLO and NADase on toxification of the host redox metabolism

    Associate Advisor

    Other advisors: Dr Stephan Brouwer, Professor Mark Walker

Completed supervision

Enquiries

Contact Professor Kate Schroder directly for media enquiries about:

  • Alzheimer's disease
  • arthritis
  • cancer
  • candida
  • caspase
  • cell biology
  • cytokine
  • diabetes
  • gout
  • hereditary disease
  • immune system
  • inerluekin
  • infection
  • infectious disease
  • inflammasome
  • inflammation
  • inflammatory disease
  • innate immunity
  • macrophage
  • myeloid
  • neutrophil
  • nod-like receptor
  • pyroptosis
  • salmonella
  • toll-like receptor

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