Solution Conformations Shed Light on PROTAC Cell Permeability

Yoseph Atilaw; Vasanthanathan Poongavanam; Caroline Svensson Nilsson; Duy Nguyen; Anja Giese; Daniel Meibom; Mate Erdelyi; Jan Kihlberg

doi:10.1021/acsmedchemlett.0c00556

Solution Conformations Shed Light on PROTAC Cell Permeability

ACS Med Chem Lett. 2020 Dec 25;12(1):107-114. doi: 10.1021/acsmedchemlett.0c00556. eCollection 2021 Jan 14.

Authors

Yoseph Atilaw¹, Vasanthanathan Poongavanam¹, Caroline Svensson Nilsson¹, Duy Nguyen², Anja Giese³, Daniel Meibom⁴, Mate Erdelyi¹, Jan Kihlberg¹

Affiliations

¹ Department of Chemistry - BMC, Uppsala University, SE-75123 Uppsala, Sweden.
² Nuvisan Innovation Campus Berlin GmbH, Muellerstrasse 178, 13353 Berlin, Germany.
³ Drug Discovery Sciences, Bayer AG, 13342 Berlin, Germany.
⁴ Drug Discovery Sciences, Bayer AG, 42113 Wuppertal, Germany.

Abstract

Proteolysis targeting chimeras (PROTACs) induce intracellular degradation of target proteins. Their bifunctional structure puts degraders in a chemical space where ADME properties often complicate drug discovery. Herein we provide the first structural insight into PROTAC cell permeability obtained by NMR studies of a VHL-based PROTAC (1), which is cell permeable despite having a high molecular weight and polarity and a large number of rotatable bonds. We found that 1 populates elongated and polar conformations in solutions that mimic extra- and intracellular compartments. Conformations were folded and had a smaller polar surface area in chloroform, mimicking a cell membrane interior. Formation of intramolecular and nonclassical hydrogen bonds, π-π interactions, and shielding of amide groups from solvent all facilitate cell permeability by minimization of size and polarity. We conclude that molecular chameleonicity appears to be of major importance for 1 to enter into target cells.