The development of phenotypic models of Parkinson's disease (PD) has enabled screening and identification of phenotypically active small molecules that restore complex biological pathways affected by PD toxicity.
The development of phenotypic models of Parkinson’s disease (PD) has enabled screening and identification of phenotypically active small molecules that restore complex biological pathways affected by PD toxicity. While these phenotypic screening platforms are powerful, they do not inherently enable direct identification of the cellular targets of promising lead compounds. To overcome this, chemoproteomic platforms like Thermal Proteome Profiling (TPP) and Stability of Proteins from Rates of Oxidation (SPROX) can be implemented to reveal protein targets of biologically active small molecules. Here we utilize both of these chemoproteomic strategies to identify targets of an N-arylbenzdiimidazole compound, NAB2, which was previously identified for its ability to restore viability in cellular models of PD-associated α-synuclein toxicity. The combined results from our TPP and SPROX analyses of NAB2 and the proteins in a neuroblastoma-derived SHSY5Y cell lysate reveal a previously unrecognized protein target of NAB2. This newly recognized target, Rab1a, is a small GTPase that acts as a molecular switch to regulate ER-to-Golgi trafficking, a process that is disrupted by α-synuclein toxicity and restored by NAB2 treatment. Further validation reveals that NAB2 binds to Rab1a with selectivity for its GDP-bound form and that NAB2 treatment phenocopies Rab1a overexpression in alleviation of α-synuclein toxicity. Finally, we conduct a preliminary investigation into the relationship between Rab1a and the E3 ubiquitin ligase, Nedd4, a previously identified NAB2 target. Together, these efforts expand our understanding of the mechanism of NAB2 in the alleviation of α-synuclein toxicity and reinforce the utility of chemoproteomic identification of the targets of phenotypically active small molecules that regulate complex biological pathways.
Disrupted
cellular trafficking and transport processes are hallmarks
of many neurodegenerative disorders (NDs). Recently, efforts have
been made toward developing and implementing experimental platforms
to identify small molecules that may help restore normative trafficking
functions. There have been a number of successes in targeting endomembrane
trafficking with the identification of compounds that restore cell
viability through rescue of protein transport and trafficking. Here,
we describe some of the experimental platforms implemented for small
molecule screening efforts for rescue of trafficking defects in neurodegeneration.
A survey of phenotypically active small molecules identified to date
is provided, including a summary of medicinal chemistry efforts and
insights into putative targets and mechanisms of action. In particular,
emphasis is put on ligands that demonstrate activity in more than
one model of neurodegeneration as retention of phenotypic activity
across ND models suggests conservation of biological targets across
NDs.
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