BiologyNature Chemistry
Selection of a promiscuous minimalist cAMP phosphodiesterase from a library of de novo designed proteins
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This groundbreaking research by J. David Schnettler and colleagues delves into how new enzyme functions can emerge from unevolved sequences. Utilizing ultrahigh-throughput droplet microfluidics, the study screens an impressive library of over one million proteins, uncovering that significant sequence changes can lead to the acquisition of activity in a newly characterized manganese-dependent metalloenzyme.
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