The dysregulation of the lysosomal degradation (autophagy) pathway has been implicated in several degenerative conditions including cancer. The development of efficient measures to control autophagy therefore potentially offers a desperately needed pathway through which cancer...
The dysregulation of the lysosomal degradation (autophagy) pathway has been implicated in several degenerative conditions including cancer. The development of efficient measures to control autophagy therefore potentially offers a desperately needed pathway through which cancer progression may be regulated. Around a quarter of deaths in Europe are currently attributed to cancer, and it is estimated that 90% of these deaths are caused by metastases. Inhibition of autophagy has recently been shown to block cell migration and prevent metastases in tumour models.
This action aims to discover a novel class of autophagy inhibitors and newly develop chemical probes that can identify their protein targets, and dissect their biological mode of action in relation to autophagy modulation.
An enabling synthetic method was developed and applied to prepare a collection of compounds that fused an sp3-rich ring system with an sp2-rich ring system (~50 compounds). These compounds are structurally related to a series of autophagy inhibitors (“oxautinsâ€) that were previously identified by the Waldmann group. The biological activity of the compounds was investigated in a range of cell-based phenotypic assays (including assays that monitor glucose uptake, hedgehog signalling, and autophagy pathways) and they were found to inhibit autophagy with sub-micromolar activity. To investigate the structure activity relationship, a further 15 analogues of the lead compound were prepared, enabling the identification of a new lead compound with nanomolar potency.
A new class of autophagy inhibitors with considerably higher potency than the originally developed compound series (“oxautinsâ€) has been realised (nM activity for the new lead compound, where only uM activity was exhibited by the previous lead compound series, oxautins). Studies will now investigate the minimum pharmacophore required for activity, as well as probe the mode of action through chemical biology techniques, in order to try to identify the molecular target(s) associated with the inhibitory activity observed. It is anticipated that the findings of this project will broadly have value towards increasing the understanding of unknown biological mechanisms underlying degenerative diseases such as cancer, which, ultimately, may aid the development of effective new treatments in future.
More info: http://www.mpi-dortmund.mpg.de/institute/directors/herbert-waldmann.