Abstract:Proteases are an important class of drug targets that
continue
to drive inhibitor discovery. These enzymes are prone to resistance
mutations, yet their promise for treating viral diseases and other
disorders continues to grow. This study develops a general approach
for detecting microbially synthesized protease inhibitors and uses
it to screen terpenoid pathways for inhibitory compounds. The detection
scheme relies on a bacterial two-hybrid (B2H) system that links protease
inactivation to the transcription of … Show more
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