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Development of subunit selective proteasome substrates for . | LitMetric

Development of subunit selective proteasome substrates for .

bioRxiv

Center for Discovery and Innovation in Parasitic Disease, Skaggs School of Pharmacy and Pharmaceutical Sciences, University of California, San Diego, 9500 Gilman Drive, La Jolla, CA 92093.

Published: February 2024

AI Article Synopsis

  • * Researchers are exploring new drug targets, specifically the 20S proteasome, which has proven successful for other parasitic infections, to find more effective treatments against schistosomiasis.
  • * By using advanced techniques like Multiplex Substrate Profiling by Mass Spectrometry, the team created optimized substrates that better measure the activity of the schistosome proteasome and found that their research could potentially benefit multiple schistosome species, leading to more efficient drug development.

Article Abstract

Schistosomiasis, or bilharzia, is a neglected tropical disease caused by spp. blood flukes that infects over 200 million people worldwide. Just one partially effective drug is available, and new drugs and drug targets would be welcome. The 20S proteasome is a validated drug target for many parasitic infections, including those caused by and . We previously showed that anticancer proteasome inhibitors that act through the 20S proteasome (Sm20S) kill the parasite . To advance these initial findings, we employed Multiplex Substrate Profiling by Mass Spectrometry (MSP-MS) to define the substrate cleavage specificities of the three catalytic β subunits of purified Sm20S. The profiles in turn were used to design and synthesize subunit-specific optimized substrates that performed two to eight fold better than the equivalent substrates used to measure the activity of the constitutive human proteasome (c20S). These specific substrates also eliminated the need to purify Sm20S from parasite extracts - a single step enrichment was sufficient to accurately measure substrate hydrolysis and its inhibition with proteasome inhibitors. Finally, we show that the substrate and inhibition profiles for the 20S proteasome from the three medically important schistosome species are similar, suggesting that data arising from an inhibitor development campaign that focuses on Sm20S can be extrapolated to the other two targets with consequent time and cost savings.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10888821PMC
http://dx.doi.org/10.1101/2024.02.13.580161DOI Listing

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