OPIG recently celebrated its 20th year; and on 10 January 2023 I gave a talk just a day before the 10th anniversary of BLOPIG’s first blog post. It’s worth reflecting on what’s stayed the same and what’s changed since then.
Continue readingTag Archives: fragments
Model validation in Crystallographic Fragment Screening
Fragment based drug discovery is a powerful technique for finding lead compounds for medicinal chemistry. Crystallographic fragment screening is particularly useful because it informs one not just about whether a fragment binds, but has the advantage of providing information on how it binds. This information allows for rational elaboration and merging of fragments.
However, this comes with a unique challenge: the confidence in the experimental readout, if and how a fragment binds, is tied to the quality of the crystallographic model that can be built. This intimately links crystallographic fragment screening to the general statistical idea of a “model”, and the statistical ideas of goodness of fit and overfitting.
Continue readingFragment-to-Lead Successes in 2019
In this blogpost, I want to highlight the excellent work by Jahnke and collaborators. For the past 5 years, they have published an annual perspective covering fragment-to-lead success stories from the previous year. Very helpfully, their work includes a table detailing the hit fragment(s) and lead molecule, together with key experimental results and parameters.
Continue readingTrying out some code from the Eighth Joint Sheffield Conference on Chemoinformatics: finding the most common functional groups present in the DSPL library
Last month a bunch of us attended the Sheffield Chemoinformatics Conference. We heard many great presentations and there were many invitations to check out one’s GitHub page. I decided now is the perfect time to try out some code that was shown by one presenter.
Peter Ertl from Novartis presented his work on the The encyclopedia of functional groups. He presented a method that automatically detects functional groups, without the use of a pre-defined list (which is what most other methods use for detecting functional groups). His method involves recursive searching through the molecule to identify groups of atoms that meet certain criteria. He used his method to answer questions such as: how many functional groups are there and what are the most common functional groups found in common synthetic molecules versus bioactive molecules versus natural products. Since I, like many others in the group, are interested in fragment libraries (possibly due to a supervisor in common), I thought I could try it out on one of these.
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