Of all the
biophysical advances so far this century, cryogenic electron microscopy (cryo-EM)
has probably made the most impressive strides. Frequently dismissed as “blobology”
just a few years ago, the technique now regularly produces three-dimensional
structural models that rival those from X-ray crystallography. Indeed, it is
rare to pick up an issue of Science or Nature that doesn’t
contain a cryo-EM structure. Earlier this year, researchers from Astex
described the structures of fragment hits against two proteins determined using
cryo-EM. Now, the boffins from DREADCO (who previously brought us universal crystallography) have begun fragment screening in cells using cryo-EM.
Fragment screening
in cells is not new: we previously highlighted work using either covalent or
non-covalent fragments. However, figuring out which proteins the fragments bind can be challenging, which is one of the reasons structural information is so
useful.
The researchers
from DREADCO incubate their fragment library against cells – human or otherwise
– for varying lengths of time. They then flash-freeze the cells in liquid
ethane, collect, and process the data, using standard cryo-EM workflows. Of
course, given the complexity of cells, the computational processing power
needed is enormous – but nothing their SkyFragNet platform can’t handle.
One of the
advantages of cryo-EM is that larger structures are more easily solved, so the
researchers are focusing on organelles such as mitochondria, as well as
ribosomes. Already they’ve found dozens of hits that resolve to high
resolution, and they are in active fragment-to-lead optimization. Surely it is
only a matter of time before our list of fragment-derived drugs includes one discovered
with the aid of cryo-EM.
🤣 Happy April 1st to you too Dan!
ReplyDeleteOh this is really good, congrats Dan!
ReplyDeleteThanks TINS1 and Till!
ReplyDeleteAnd while this was in fact our twelfth consecutive April Fools' post, I wasn't jesting about the impressive strides cryo-EM has made. Indeed, Nobel Laureate Richard Henderson recently stated that by 2024 "more protein structures will be determined by cryo-EM than by X-ray crystallography." So I hold with my prediction that "it is only a matter of time before our list of fragment-derived drugs includes one discovered with the aid of cryo-EM"