Structural and conformational determinants of macrocycle cell permeability.

نویسندگان

  • Björn Over
  • Pär Matsson
  • Christian Tyrchan
  • Per Artursson
  • Bradley C Doak
  • Michael A Foley
  • Constanze Hilgendorf
  • Stephen E Johnston
  • Maurice D Lee
  • Richard J Lewis
  • Patrick McCarren
  • Giovanni Muncipinto
  • Ulf Norinder
  • Matthew W D Perry
  • Jeremy R Duvall
  • Jan Kihlberg
چکیده

Macrocycles are of increasing interest as chemical probes and drugs for intractable targets like protein-protein interactions, but the determinants of their cell permeability and oral absorption are poorly understood. To enable rational design of cell-permeable macrocycles, we generated an extensive data set under consistent experimental conditions for more than 200 non-peptidic, de novo-designed macrocycles from the Broad Institute's diversity-oriented screening collection. This revealed how specific functional groups, substituents and molecular properties impact cell permeability. Analysis of energy-minimized structures for stereo- and regioisomeric sets provided fundamental insight into how dynamic, intramolecular interactions in the 3D conformations of macrocycles may be linked to physicochemical properties and permeability. Combined use of quantitative structure-permeability modeling and the procedure for conformational analysis now, for the first time, provides chemists with a rational approach to design cell-permeable non-peptidic macrocycles with potential for oral absorption.

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عنوان ژورنال:
  • Nature chemical biology

دوره 12 12  شماره 

صفحات  -

تاریخ انتشار 2016