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Lipophilic Permeability Efficiency Reconciles the Opposing Roles of Lipophilicity in Membrane Permeability and Aqueous Solubility.
Naylor, Matthew R; Ly, Andrew M; Handford, Mason J; Ramos, Daniel P; Pye, Cameron R; Furukawa, Akihiro; Klein, Victoria G; Noland, Ryan P; Edmondson, Quinn; Turmon, Alexandra C; Hewitt, William M; Schwochert, Joshua; Townsend, Chad E; Kelly, Colin N; Blanco, Maria-Jesus; Lokey, R Scott.
Affiliation
  • Naylor MR; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Ly AM; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Handford MJ; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Ramos DP; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Pye CR; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Furukawa A; Modality Research Laboratories , Daiichi Sankyo Company, Ltd. , 1-2-58 Hiromachi , Shingawa-ku, Tokyo 140-8710 , Japan.
  • Klein VG; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Noland RP; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Edmondson Q; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Turmon AC; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Hewitt WM; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Schwochert J; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Townsend CE; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Kelly CN; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
  • Blanco MJ; Sage Therapeutics , 215 First Street, Suite 220 , Cambridge , Massachusetts 02142 , United States.
  • Lokey RS; Department of Chemistry and Biochemistry , University of California Santa Cruz , 1156 High Street , Santa Cruz , California 95064 , United States.
J Med Chem ; 61(24): 11169-11182, 2018 12 27.
Article in En | MEDLINE | ID: mdl-30395703
As drug discovery moves increasingly toward previously "undruggable" targets such as protein-protein interactions, lead compounds are becoming larger and more lipophilic. Although increasing lipophilicity can improve membrane permeability, it can also incur serious liabilities, including poor water solubility, increased toxicity, and faster metabolic clearance. Here we introduce a new efficiency metric, especially relevant to "beyond rule of 5" molecules, that captures, in a simple, unitless value, these opposing effects of lipophilicity on molecular properties. Lipophilic permeability efficiency (LPE) is defined as log D7.4dec/w - mlipocLogP + bscaffold, where log D7.4dec/w is the experimental decadiene-water distribution coefficient (pH 7.4), cLogP is the calculated octanol-water partition coefficient, and mlipo and bscaffold are scaling factors to standardize LPE values across different cLogP metrics and scaffolds. Using a variety of peptidic and nonpeptidic macrocycle drugs, we show that LPE provides a functional assessment of the efficiency with which a compound achieves passive membrane permeability at a given lipophilicity.
Subject(s)

Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Structure-Activity Relationship / Pharmaceutical Preparations / Cell Membrane Permeability Language: En Journal: J Med Chem Journal subject: QUIMICA Year: 2018 Document type: Article Affiliation country: United States Country of publication: United States

Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Structure-Activity Relationship / Pharmaceutical Preparations / Cell Membrane Permeability Language: En Journal: J Med Chem Journal subject: QUIMICA Year: 2018 Document type: Article Affiliation country: United States Country of publication: United States