The Hedgehog (Hh) pathway is a conserved cell-cell signalling pathway that is normally involved in the development of tissue, but is associated with cancer during maturity. There is strong evidence that Hh signalling plays an important role in pancreatic ductal adenocarcinoma (PDAC), a very deadly (5-year survival rate is 5%) form of cancer, as well as being involved in over 25% of cancer deaths. however, the Hh pathway is highly complex and includes several poorly understood branches. Nevertheless, completely removing Hh signalling has been shown to effectively inhibit PDAC growth. Approved Hh inhibitors Vismodegib and Sonidegib exist, but are not effective against PDAC because they do not completely inhibit Hh signalling. We propose developing alternative Hh targeting drugs that are capable of completely inhibiting Hh signalling, thus providing the tool compounds to start developing a drug against this deadly disease, and cancer more generally. Our approach is based on targeting the protein Hedgehog acyltransferase (HHAT), a critical protein in the Hh pathway. The overall objective of the project is to generate compounds that have the right potency and physicochemical properties to target HHAT in cells and animal models. This objective has been achieved, as we have generated a molecule that has high potency against HHAT, good stability, as well as being well tolerated in mice.