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Pancrea_tive-T

  • Research type

    Research Study

  • Full title

    Analysis of tumour-stroma heterogeneity in human pancreatic cancer

  • IRAS ID

    317488

  • Contact name

    Stephen Kelleher

  • Contact email

    research@addebrookes.nhs.uk

  • Sponsor organisation

    Cambridge University Hospitals NHS Foundation Trust and the University of Cambridge

  • Duration of Study in the UK

    3 years, 3 months, 2 days

  • Research summary

    Pancreatic cancer is highly lethal, with only 1 in 10 patients surviving the first 5 years. Pancreatic tumours are complex consisting of tumour cells along with other cell types, such as fibroblasts and immune cells along with a dense, fibrous matrix collectively called stroma. This stroma can make up to 90% of the tumour, and makes tumours resistant to treatment.
    Within the stroma, fibroblasts are the most abundant cell type. There are different types of fibroblasts, and their
    contribution to tumour growth and treatment resistance is poorly understood. There is evidence to suggest that some types of fibroblasts increase tumour growth and drug resistance, and others have the opposite effect. Therefore, we aim to understand how cancer cells and fibroblasts interact and affect each other.
    To address this, we have developed model systems in the lab, including mouse pancreatic tumour organoid/fibroblast co-cultures and mouse models that largely mimic human PDAC. In combination with these models, we use drugs and genetic approaches to characterise the roles and dynamic nature of the different types of fibroblasts during different stages of pancreatic cancer progression. Although laboratory models have so far been instrumental in our understanding of pancreatic tumours, we still have limited information about the composition of the pancreatic cancer microenvironment in human PDAC. To this end, the analysis of patient samples will be essential to advance our knowledge of the roles of fibroblasts and to identify new potential targets for treatment. Altogether, our studies will determine how different fibroblast types interact with other cell types in the tumour and support pancreatic cancer progression. This analysis will help identify new treatments/combinations to selectively target the fibroblasts that promote tumour growth.

  • REC name

    East of England - Cambridge South Research Ethics Committee

  • REC reference

    22/EE/0223

  • Date of REC Opinion

    4 Nov 2022

  • REC opinion

    Further Information Favourable Opinion

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