Methods for the Analysis of Matched Molecular Pairs and Chemical Space Representations

Compound optimization is a complex process where different properties are optimized to increase the biological activity and therapeutic effects of a molecule. Frequently, the structure of molecules is modified in order to improve their property values. Therefore, computational analysis of the effects of structure modifications on property values is of great importance for the drug discovery process. It is also essential to analyze chemical space, i.e., the set of all chemically feasible molecules, in order to find subsets of molecules that display favorable property values. This thesis aims to expand the computational repertoire to analyze the effect of structure alterations and visualize chemical space. Matched molecular pairs are defined as pairs of compounds that share a large common substructure and only differ by a small chemical transformation. They have been frequently used to study property changes caused by structure modifications. These analyses are expanded in this thesis by studying the effect of chemical transformations on the ionization state and ligand efficiency, both measures of great importance in drug design. Additionally, novel matched molecular pairs based on retrosynthetic rules are developed to increase their utility for prospective use of chemical transformations in compound optimization. Further, new methods based on matched molecular pairs are described to obtain preliminary SAR information of screening hit compounds and predict the potency change caused by a chemical transformation. Visualizations of chemical space are introduced to aid compound optimization efforts. First, principal component plots are used to rationalize a matched molecular pair based multi-objective compound optimization procedure. Then, star coordinate and parallel coordinate plots are introduced to analyze drug-like subspaces, where compounds with favorable property values can be found. Finally, a novel network-based visualization of high-dimensional property space is developed. Concluding, the applications developed in this thesis expand the methodological spectrum of computer-aided compound optimization

Computational Methods Generating High-Resolution Views of Complex Structure-Activity Relationships

The analysis of structure-activity relationships (SARs) of small bioactive compounds is a central task in medicinal chemistry and pharmaceutical research. The study of SARs is in principle not limited to computational methods, however, as data sets rapidly grow in size, advanced computational approaches become indispensable for SAR analysis. Activity landscapes are one of the preferred and widely used computational models to study large-scale SARs. Activity cliffs are cardinal features of activity landscape representations and are thought to contain high SAR information content. This work addresses major challenges in systematic SAR exploration and specifically focuses on the design of novel activity landscape models and comprehensive activity cliff analysis. In the first part of the thesis, two conceptually different activity landscape representations are introduced for compounds active against multiple targets. These models are designed to provide an intuitive graphical access to compounds forming single and multi-target activity cliffs and displaying multi-target SAR characteristics. Further, a systematic analysis of the frequency and distribution of activity cliffs is carried out. In addition, a large-scale data mining effort is designed to quantify and analyze fingerprint-dependent changes in SAR information. The second part of this work is dedicated to the concept of activity cliffs and their utility in the practice of medicinal chemistry. Therefore, a computational approach is introduced to search for detectable SAR advantages associated with activity cliffs. In addition, the question is investigated to what extent activity cliffs might be utilized as starting points in practical compound optimization efforts. Finally, all activity cliff configurations formed by currently available bioactive compounds are thoroughly examined. These configurations are further classified and their frequency of occurrence and target distribution are determined. Furthermore, the activity cliff concept is extended to explore the relation between chemical structures and compound promiscuity. The notion of promiscuity cliffs is introduced to deduce structural modifications that might induce large-magnitude promiscuity effects