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| Funder | Wellcome Trust |
|---|---|
| Recipient Organization | MRC Laboratory of Molecular Biology |
| Country | United Kingdom |
| Start Date | Jan 01, 2024 |
| End Date | Dec 31, 2031 |
| Duration | 2,921 days |
| Number of Grantees | 1 |
| Roles | Award Holder |
| Data Source | Europe PMC |
| Grant ID | 226525 |
Wnt signalling pathways orchestrate a multitude of fundamental biological processes, including cell fate determination and differentiation during embryonic development. The overwhelming majority of Wnt research has focussed on the canonical Wnt/b-catenin pathway.
By contrast, the non-canonical Wnt/ROR pathway, which constitutes a core developmental pathway that controls tissue morphogenesis during development, remains poorly characterised.
Dysfunction of the Wnt/ROR pathway causes several rare genetic diseases and is implicated in neurological disorders and in driving the metastatic progression of many cancers.
Therefore, defining the Wnt/ROR signalling pathway mechanistically is essential to develop better more targeted therapies and impact human health.
My vision is to transform our understanding of the crucial Wnt/ROR pathway and elucidate how its misregulation drives developmental disease.
My starting focus is on Wnt/ROR signalosomes, which are dynamic multiprotein complexes whose function and components require elucidation.
I will use wildtype and disease-associated mutants in proximity labelling proteomic assays to systemically identify novel Wnt/ROR signalling partners.
This will be combined with biochemical assays to define their direct interactions and innovative cell-based functional assays to determine those that are essential for signalling.
I will determine: (1) Wnt/ROR signalosome components (2) ROR- receptor pseudokinase signalling mechanisms and (3) uncover how Wnt/ROR abnormalities cause developmental diseases.
MRC Laboratory of Molecular Biology
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