Replacement of dichloromethane within chromatographic purification : a guide to alternative solvents

Replacement of dichloromethane as the bulk medium within chromatographic purification has been evaluated with a broad range of molecules containing functionality common within Medicinal Chemistry programmes. Analysis of the data set has generated a set of general guidelines to assist in the selection of alternative solvents for CH2Cl2 as the bulk media in these ubiquitously employed processes

Neutral genetic drift can aid functional protein evolution

BACKGROUND: Many of the mutations accumulated by naturally evolving proteins are neutral in the sense that they do not significantly alter a protein's ability to perform its primary biological function. However, new protein functions evolve when selection begins to favor other, "promiscuous" functions that are incidental to a protein's biological role. If mutations that are neutral with respect to a protein's primary biological function cause substantial changes in promiscuous functions, these mutations could enable future functional evolution. RESULTS: Here we investigate this possibility experimentally by examining how cytochrome P450 enzymes that have evolved neutrally with respect to activity on a single substrate have changed in their abilities to catalyze reactions on five other substrates. We find that the enzymes have sometimes changed as much as four-fold in the promiscuous activities. The changes in promiscuous activities tend to increase with the number of mutations, and can be largely rationalized in terms of the chemical structures of the substrates. The activities on chemically similar substrates tend to change in a coordinated fashion, potentially providing a route for systematically predicting the change in one function based on the measurement of several others. CONCLUSIONS: Our work suggests that initially neutral genetic drift can lead to substantial changes in protein functions that are not currently under selection, in effect poising the proteins to more readily undergo functional evolution should selection "ask new questions" in the future

Computational Analysis of Structure-Activity Relationships : From Prediction to Visualization Methods

Understanding how structural modifications affect the biological activity of small molecules is one of the central themes in medicinal chemistry. By no means is structure-activity relationship (SAR) analysis a priori dependent on computational methods. However, as molecular data sets grow in size, we quickly approach our limits to access and compare structures and associated biological properties so that computational data processing and analysis often become essential. Here, different types of approaches of varying complexity for the analysis of SAR information are presented, which can be applied in the context of screening and chemical optimization projects. The first part of this thesis is dedicated to machine-learning strategies that aim at de novo ligand prediction and the preferential detection of potent hits in virtual screening. High emphasis is put on benchmarking of different strategies and a thorough evaluation of their utility in practical applications. However, an often claimed disadvantage of these prediction methods is their "black box" character because they do not necessarily reveal which structural features are associated with biological activity. Therefore, these methods are complemented by more descriptive SAR analysis approaches showing a higher degree of interpretability. Concepts from information theory are adapted to identify activity-relevant structure-derived descriptors. Furthermore, compound data mining methods exploring prespecified properties of available bioactive compounds on a large scale are designed to systematically relate molecular transformations to activity changes. Finally, these approaches are complemented by graphical methods that primarily help to access and visualize SAR data in congeneric series of compounds and allow the formulation of intuitive SAR rules applicable to the design of new compounds. The compendium of SAR analysis tools introduced in this thesis investigates SARs from different perspectives

Application of the SwissDrugDesign Online Resources in Virtual Screening.

SwissDrugDesign is an important initiative led by the Molecular Modeling Group of the SIB Swiss Institute of Bioinformatics. This project provides a collection of freely available online tools for computer-aided drug design. Some of these web-based methods, i.e., SwissSimilarity and SwissTargetPrediction, were especially developed to perform virtual screening, while others such as SwissADME, SwissDock, SwissParam and SwissBioisostere can find applications in related activities. The present review aims at providing a short description of these methods together with examples of their application in virtual screening, where SwissDrugDesign tools successfully supported the discovery of bioactive small molecules