Download
1 / 26
E N D
Slide 21:An example – BioFocus library TPF11
large library (ca. >700 compounds) based on two cores and 9 scaffolds extensively elaborated at a single position so that the scaffold becomes the effective second variable. These compounds are not reported in SciFinder or by commercial supplier
Lead optimisation – where (medchem) going gets tough! Balance of activities – into the nearly-unknown; until more data are available from network biomarker and enzyme-occupancy studies, balanced potency is the best guess – very high multipotency may well not be required Balance of physicochemical properties – tricky for MKIs where structural additivity tends to correlate with selectivity – however, deliberate choice of overlapping pharmacophores helps; non-oncology applications are more challenging Balance of off-target activities – this issue is no different in principle to that for so-called “selective” kinase inhibitors, of which there are not many. Isolated enzyme assays are, at best, an approximate guide to undesirable intra-family activities. Monitoring cellular target/s activity against in vitro and in vivo toxicity readouts are essential in lead optimisation. Facilitating parallel lead optimisation Parallel optimisation is the ideal: This is the area of greatest current medchem caution! Lead optimisation against more than one non-ADMET/PK target is somewhat foreign to current practice, at least outside the kinase area. Biochemical and cellular kinase assays need to be run in close conjunction with each other, even more so than for “monovalent” kinase inhibitors – HCS technologies are beginning to impact optimisation in this way. Cellular assays can also measure inhibitory mechanisms which are missed by current biochemical methods Cross-target SARs are, by their nature, more complex than single-target SARs and compromises are generally to be expected Therefore it is very important to qualify these SAR compromises, preferably in cellular disease models or even primary cells In Oncology MKIs will become the norm in the kinase inhibitor field; combination therapy and MTDs with kinase and synergising non-kinase drugs will emerge In Inflammation Certain MKIs will make it to clinic and safety assessments will be very interesting. For example, Palau have DD-2, a dual Jak3/Syk inhibitor in preclinical for autoimmune diseases and there are unpublished data for related approaches Whither other complex multifaceted diseases? Additional references “Network pharmacology: the next paradigm in drug discovery”, A L Hopkins, Nature Chemical Biology, 2008, 682. “What does Systems Biology mean for drug discovery” A Schrattenholz, Vukic Soskic, Current Medicinal Chemistry, 2008, 1520. “Designed Multiple Ligands. An emerging drug discovery paradigm” Richard Morphy, Zoran Rankovic, J Med. Chem., 2005, 6523. “The physicochemical challenges of designing multiple ligands” Richard Morphy, Zoran Rankovic, J Med. Chem., 2006, 4961. “Logic models of pathway biology”, Steven Watterson, Stephen Marshall, Peter Ghazal, Drug Discovery Today, 2008, 447. “Can we rationally design promiscuous drugs” A L Hopkins, J S Mason, J Overington, Current Opinion in Structural Biology, 2006, 127. “Discovery of multitarget inhibitors by combining molecular docking with common pharmacophore features” D Wei, X Jiang, L Zhou, J Chen, Z Chen, C He, K Yang, Y Liu, J Pei, L Lai, J Med. Chem., 2008, 7882. “Selectively Nonselective Kinase Inhibition: Striking the Right Balance” R Morphy, J Med Chem.,.2010, 1413. Acknowledgements for helpful discussions: Richard Morphy (Schering-Plough) Kate Hilyard, Chris Newton (BioFocus) Ian James (Almac Biosciences) John Overington (EMBL Cambridge) Colin Telfer, Finbarr Murphy (Lee Oncology)
