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1. A super-potent tetramerized ACE2 protein displays enhanced neutralization of SARS-CoV-2 virus infection

2. Implementing a method for engineering multivalency to substantially enhance binding of clinical trial anti-SARS-CoV-2 antibodies to wildtype spike and variants of concern proteins

3. Fragment-based screening maps inhibitor interactions in the ATP-binding site of checkpoint kinase 2.

4. iTAG an optimized IMiD-induced degron for targeted protein degradation in human and murine cells

5. Discovery of an In Vivo Chemical Probe for BCL6 Inhibition by Optimization of Tricyclic Quinolinones

6. Discovery of 2-(3-Benzamidopropanamido)thiazole-5-carboxylate Inhibitors of the Kinesin HSET (KIFC1) and the Development of Cellular Target Engagement Probes

7. Optimizing Shape Complementarity Enables the Discovery of Potent Tricyclic BCL6 Inhibitors

8. Improved Binding Affinity and Pharmacokinetics Enable Sustained Degradation of BCL6 In Vivo

9. Supplementary Fig 6 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

10. Supplementary Tables S1-S10 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

11. Supplementary Fig 2 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

12. Supplementary Fig 3 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

13. Supplementary experimental procedures figure legends and references from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

15. Supplementary Fig 1 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

17. Into Deep Water: Optimizing BCL6 Inhibitors by Growing into a Solvated Pocket

18. Discovering cell-active BCL6 inhibitors: effectively combining biochemical HTS with multiple biophysical techniques, X-ray crystallography and cell-based assays

19. Achieving In Vivo Target Depletion through the Discovery and Optimization of Benzimidazolone BCL6 Degraders

20. Application of a Method for Engineering Multivalent Antibodies to Substantially Enhance Functional affinity of Clinical Trial Anti-SARS-CoV-2 Antibodies

21. Achieving

22. Structural and functional characterisation of human RNA helicase DHX8 provides insights into the mechanism of RNA-stimulated ADP release

23. Demonstrating In-Cell Target Engagement Using a Pirin Protein Degradation Probe (CCT367766)

24. Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

25. A fragment-based approach applied to a highly flexible target: Insights and challenges towards the inhibition of HSP70 isoforms

26. Identification of Autophosphorylation Inhibitors of the Inositol-Requiring Enzyme 1 Alpha (IRE1α) by High-Throughput Screening Using a DELFIA Assay

27. Detection of the ATPase Activity of the Molecular Chaperones Hsp90 and Hsp72 Using the Transcreener™ ADP Assay Kit

28. Structure-based design of orally bioavailable 1H-pyrrolo[3,2-c]pyridine inhibitors of mitotic kinase monopolar spindle 1 (MPS1)

29. Fragment-based screening maps inhibitor interactions in the ATP-binding site of checkpoint kinase 2

30. Abstract 2843: Resistance to ERK inhibitors as a result of an acquired novel P-loop mutation of ERK2

31. Abstract 5450: Naturally occurring mutations in the MPS1 gene predispose cells to kinase inhibitor drug-resistance

32. Abstract 3242: CCT271850, a novel, selective, highly potent and orally bioavailable Mps1 kinase inhibitor

33. Development and evaluation of selective, reversible LSD1 inhibitors derived from fragments

34. Abstract 1817: Characterisation of CCT251455, a novel, selective and highly potent Mps1 kinase inhibitor

35. Abstract A239: MPS1 (TTK) kinase inhibition selectively kills aneuploid cells

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