论文信息 - Evaluation of dynamic polar molecular surface area as predictor of drug absorption: comparison with other computational and experimental predictors. - 字舞流文

Evaluation of dynamic polar molecular surface area as predictor of drug absorption: comparison with other computational and experimental predictors.

The relationship between various molecular descriptors and transport of drugs across the intestinal epithelium was evaluated. The monolayer permeability (Pc) of human intestinal Caco-2 cells to a series of nine beta-receptor-blocking agents was investigated in vitro. The dynamic polar molecular surface area (PSAd) of the compounds was calculated from all low-energy conformations identified in molecular mechanics calculations in vacuum and in simulated chloroform and water environments. For most of the investigated drugs, the effects of the different environments on PSAd were small. The exception was H 216/44, which is a large flexible compound containing several functional groups capable of hydrogen bonding (PSAd,chloroform = 70.8 A2 and PSAd,water = 116.6 A2). The relationship between Pc and PSAd was stronger than those between Pc and the calculated octanol/water distribution coefficients (log Dcalc) or the experimentally determined immobilized liposome chromatography (ILC) retention. Pc values for two new practolol analogues and H 216/44 were predicted from the structure-permeability relationships of a subset of the nine compounds and compared with experimental values. The Pc values of the two practolol analogues were predicted well from both PSAd calculations and ILC retention studies. The Pc value of H 216/44 was reasonably well-predicted only from the PSAd of conformations preferred in vacuum and in water. The other descriptors overestimated the Pc of H 216/44 100-500-fold.

K. Luthman | P. Artursson | A. Ungell | K. Palm | G. Strandlund | P Artursson | K Palm | K Luthman | P. Lundahl | A L Ungell | G Strandlund | F Beigi | P Lundahl | F. Beigi | Kristina Luthman | Gert Strandlund | Farideh Beigi | Per Lundahl | Per Artursson | Katrin Palm

[1] R. Schoenwald,et al. Corneal penetration behavior of beta-blocking agents I: Physiochemical factors. , 1983, Journal of pharmaceutical sciences.

[2] Y. Martin,et al. A practitioner's perspective of the role of quantitative structure-activity analysis in medicinal chemistry. , 1981, Journal of medicinal chemistry.

[3] Raimund Mannhold,et al. Drug lipophilicity in QSAR practice. I: A comparison of experimental with calculative approaches , 1990 .

[4] K. Luthman,et al. Correlation of drug absorption with molecular surface properties. , 1996, Journal of pharmaceutical sciences.

[5] E. Brekkan,et al. Immobilized liposome and biomembrane partitioning chromatography of drugs for prediction of drug transport , 1998 .

[6] A. Lundqvist,et al. Freeze–thaw immobilization of liposomes in chromatographic gel beads: evaluation by confocal microscopy and effects of freezing rate , 1998, Journal of molecular recognition : JMR.

[7] R Griffiths,et al. Development of a new physicochemical model for brain penetration and its application to the design of centrally acting H2 receptor histamine antagonists. , 1988, Journal of medicinal chemistry.

[8] W J Dunn,et al. The role of solvent-accessible surface area in determining partition coefficients. , 1987, Journal of medicinal chemistry.

[9] R. Borchardt,et al. How structural features influence the biomembrane permeability of peptides. , 1996, Journal of pharmaceutical sciences.

[10] N el Tayar,et al. Partitioning of solutes in different solvent systems: the contribution of hydrogen-bonding capacity and polarity. , 1991, Journal of pharmaceutical sciences.

[11] P. Artursson,et al. Correlation between oral drug absorption in humans and apparent drug permeability coefficients in human intestinal epithelial (Caco-2) cells. , 1991, Biochemical and biophysical research communications.

[12] Samuel H. Yalkowsky,et al. Solubility of nonelectrolytes in polar solvents. V. Estimation of the solubility of aliphatic monofunctional compounds in water using a molecular surface area approach , 1975 .

[13] C Silipo,et al. Calculation of hydrophobic constant (log P) from pi and f constants. , 1975, Journal of medicinal chemistry.

[14] P. Artursson,et al. Epithelial transport of drugs in cell culture. VII: Effects of pharmaceutical surfactant excipients and bile acids on transepithelial permeability in monolayers of human intestinal epithelial (Caco-2) cells. , 1992, Journal of pharmaceutical sciences.

[15] H. Scheraga,et al. Accessible surface areas as a measure of the thermodynamic parameters of hydration of peptides. , 1987, Proceedings of the National Academy of Sciences of the United States of America.

[16] G. Chang,et al. Macromodel—an integrated software system for modeling organic and bioorganic molecules using molecular mechanics , 1990 .

[17] D. Scherman,et al. High lipophilicity decreases drug transport across intestinal epithelial cells. , 1994, The Journal of pharmacology and experimental therapeutics.

[18] M. Kansy,et al. Hydrogen-Bonding Capacity and Brain Penetration , 1992, Chimia (Basel).

[19] Kenny B. Lipkowitz,et al. Dynamic molecular surface areas , 1989 .

[20] B. Lee,et al. The interpretation of protein structures: estimation of static accessibility. , 1971, Journal of molecular biology.

[21] P. Artursson,et al. Transport of celiprolol across human intestinal epithelial (Caco‐2) cells: mediation of secretion by multiple transporters including P‐glycoprotein , 1993, British journal of pharmacology.

[22] Q. Yang,et al. Immobilized-liposome chromatographic analysis of drug partitioning into lipid bilayers. , 1995, Journal of chromatography. A.

[23] C. Joyce. Drug Compendium , 1970, Nature.

[24] R. Schoenwald,et al. Corneal Penetration Behavior of β-Blocking Agents I: Physicochemical Factors , 1983 .

[25] D. Barlow,et al. The design of peptide analogues for improved absorption , 1994 .

[26] C. Pidgeon,et al. IAM chromatography: an in vitro screen for predicting drug membrane permeability. , 1995, Journal of medicinal chemistry.

[27] P. Artursson,et al. Epithelial transport of drugs in cell culture. I: A model for studying the passive diffusion of drugs over intestinal absorptive (Caco-2) cells. , 1990, Journal of pharmaceutical sciences.

[28] H. Lennernäs,et al. Comparison between active and passive drug transport in human intestinal epithelial (Caco-2) cells in vitro and human jejunum in vivo , 1996 .

[29] Alex Avdeef,et al. pH‐Metric log P. Part 1. Difference Plots for Determining Ion‐Pair Octanol‐Water Partition Coefficients of Multiprotic Substances , 1992 .

[30] J. Taskinen,et al. Relationship between immobilised artificial membrane chromatographic retention and the brain penetration of structurally diverse drugs. , 1997, Journal of pharmaceutical and biomedical analysis.

[31] Han van de Waterbeemd,et al. Estimation of Caco‐2 Cell Permeability using Calculated Molecular Descriptors , 1996 .

[32] W. Rubas,et al. Structural Elements Which Govern the Resistance of Intestinal Tissues to Compound Transport , 1993 .

[33] P. Artursson,et al. A method for the determination of cellular permeability coefficients and aqueous boundary layer thickness in monolayers of intestinal epithelial caco 2 cells grown in permeable filter chambers , 1991 .

[34] S H White,et al. The nature of the hydrophobic binding of small peptides at the bilayer interface: implications for the insertion of transbilayer helices. , 1989, Biochemistry.