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Title: Rational Design of Orthogonal Multipolar Interactions with Fluorine in Protein–Ligand Complexes

Journal Article · · Journal of Medicinal Chemistry
 [1];  [1];  [1];  [1];  [2];  [1];  [1]
  1. Univ. of Michigan, Ann Arbor, MI (United States). Dept. of Pathology
  2. Wroclaw Univ. of Technology (Poland). Dept. of Chemistry
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Multipolar interactions involving fluorine and the protein backbone have been frequently observed in protein–ligand complexes. Such fluorine–backbone interactions may substantially contribute to the high affinity of small molecule inhibitors. Here we found that introduction of trifluoromethyl groups into two different sites in the thienopyrimidine class of menin–MLL inhibitors considerably improved their inhibitory activity. In both cases, trifluoromethyl groups are engaged in short interactions with the backbone of menin. In order to understand the effect of fluorine, we synthesized a series of analogues by systematically changing the number of fluorine atoms, and we determined high-resolution crystal structures of the complexes with menin. Here, we found that introduction of fluorine at favorable geometry for interactions with backbone carbonyls may improve the activity of menin–MLL inhibitors as much as 5- to 10-fold. In order to facilitate the design of multipolar fluorine–backbone interactions in protein–ligand complexes, we developed a computational algorithm named FMAP, which calculates fluorophilic sites in proximity to the protein backbone. We demonstrated that FMAP could be used to rationalize improvement in the activity of known protein inhibitors upon introduction of fluorine. Furthermore, FMAP may also represent a valuable tool for designing new fluorine substitutions and support ligand optimization in drug discovery projects. Analysis of the menin–MLL inhibitor complexes revealed that the backbone in secondary structures is particularly accessible to the interactions with fluorine. Lastly, considering that secondary structure elements are frequently exposed at protein interfaces, we postulate that multipolar fluorine–backbone interactions may represent a particularly attractive approach to improve inhibitors of protein–protein interactions.

Research Organization:
Argonne National Laboratory (ANL), Argonne, IL (United States). Advanced Photon Source (APS)
Sponsoring Organization:
USDOE Office of Science (SC)
Grant/Contract Number:
AC02-06CH11357; 085P1000817; RSG-11-082-01-DMC; 6116-12; RSG-13-130-01-CDD; R01 CA181185; R01 CA160467
OSTI ID:
1222005
Journal Information:
Journal of Medicinal Chemistry, Vol. 58, Issue 18; ISSN 0022-2623
Publisher:
American Chemical Society (ACS)Copyright Statement
Country of Publication:
United States
Language:
ENGLISH
Citation Metrics:
Cited by: 55 works
Citation information provided by
Web of Science

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Cited By (11)

Regulation of Protein Activity and Cellular Functions Mediated by Molecularly Evolved Nucleic Acids journal January 2019
Study of Fluorinated Quantum Dots-Protein Interactions at the Oil/Water Interface by Interfacial Surface Tension Changes journal May 2018
Using Structural Analysis In Silico to Assess the Impact of Missense Variants in MEN1 journal September 2019
Taking Advantage of Hydrophobic Fluorine Interactions for Self-Assembled Quantum Dots as a Delivery Platform for Enzymes journal March 2018
Are fluorine-based contacts predictable? A case study in three similar coordination compounds journal January 2017
Structure and Energetics of Ligand–Fluorine Interactions with Galectin‐3 Backbone and Side‐Chain Amides: Insight into Solvation Effects and Multipolar Interactions journal July 2019
A systematic analysis of atomic protein–ligand interactions in the PDB journal January 2017
Regulation of Protein Activity and Cellular Functions Mediated by Molecularly Evolved Nucleic Acids journal January 2019
Taking Advantage of Hydrophobic Fluorine Interactions for Self-Assembled Quantum Dots as a Delivery Platform for Enzymes journal March 2018
Harnessing Fluorine–Sulfur Contacts and Multipolar Interactions for the Design of p53 Mutant Y220C Rescue Drugs journal June 2016
Dissecting the Structure–Activity Relationship of Galectin–Ligand Interactions journal January 2018

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