The solubility-permeability interplay and oral drug formulation design: Two heads are better than one

被引:152
作者
Dahan, Arik [1 ]
Beig, Avital [1 ]
Lindley, David [2 ]
Miller, Jonathan M. [2 ,3 ]
机构
[1] Ben Gurion Univ Negev, Fac Hlth Sci, Dept Clin Pharmacol, Sch Pharm, IL-84105 Beer Sheva, Israel
[2] AbbVie Inc, Abbott Pk, IL 60064 USA
[3] Vertex Pharmaceut, 50 Northern Ave, Boston, MA 02210 USA
关键词
Biopharmaceutics Classification System (BCS); Drug solubility; Intestinal permeability; Solubility-enabling formulations; Solubility permeability tradeoff; WATER-SOLUBLE DRUGS; LIPID-BASED FORMULATIONS; IN-VIVO BIOAVAILABILITY; BILE-ACID SURFACTANTS; ENABLING FORMULATIONS; INTESTINAL PERMEABILITY; MEMBRANE-TRANSPORT; DELIVERY-SYSTEMS; XENOBIOTIC ABSORPTION; LIPOPHILIC DRUGS;
D O I
10.1016/j.addr.2016.04.018
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Poor aqueous solubility is a major challenge in today's biopharmaceutics. While solubility-enabling formulations can significantly increase the apparent solubility of the drug, the concomitant effect on the drug's apparent permeability has been largely overlooked. The mathematical equation to describe the membrane permeability of a drug comprises the membrane/aqueous partition coefficient, which in turn is dependent on the drug's apparent solubility in the GI milieu, suggesting that the solubility and the permeability are closely related, exhibit a certain interplay between them, and treating the one irrespectively of the other may be insufficient. In this article, an overview of this solubility-permeability interplay is provided, and the available data is analyzed in the context of the effort to maximize the overall drug exposure. Overall, depending on the type of solubility-permeability interplay, the permeability may decrease, remain unchanged, and even increase, in a way that may critically affect the formulation capability to improve the overall absorption. Therefore, an intelligent design of solubility-enabling formulation needs to consider both the solubility afforded by the formulation and the permeability in the new luminal environment resulting from the formulation. (C) 2016 Elsevier B.V. All rights reserved.
引用
收藏
页码:99 / 107
页数:9
相关论文
共 87 条
[1]   THEORETICAL AND EXPERIMENTAL STUDIES OF TRANSPORT OF MICELLE-SOLUBILIZED SOLUTES [J].
AMIDON, GE ;
HIGUCHI, WI ;
HO, NFH .
JOURNAL OF PHARMACEUTICAL SCIENCES, 1982, 71 (01) :77-84
[2]   A THEORETICAL BASIS FOR A BIOPHARMACEUTIC DRUG CLASSIFICATION - THE CORRELATION OF IN-VITRO DRUG PRODUCT DISSOLUTION AND IN-VIVO BIOAVAILABILITY [J].
AMIDON, GL ;
LENNERNAS, H ;
SHAH, VP ;
CRISON, JR .
PHARMACEUTICAL RESEARCH, 1995, 12 (03) :413-420
[3]   Evaluation of amorphous solid dispersion properties using thermal analysis techniques [J].
Baird, Jared A. ;
Taylor, Lynne S. .
ADVANCED DRUG DELIVERY REVIEWS, 2012, 64 (05) :396-421
[4]   Head-To-Head Comparison of Different Solubility-Enabling Formulations of Etoposide and Their Consequent Solubility-Permeability Interplay [J].
Beig, Avital ;
Miller, Jonathan M. ;
Lindley, David ;
Carr, Robert A. ;
Zocharski, Philip ;
Agbaria, Riad ;
Dahan, Arik .
JOURNAL OF PHARMACEUTICAL SCIENCES, 2015, 104 (09) :2941-2947
[5]   The use of captisol (SBE7-β-CD) in oral solubility-enabling formulations: Comparison to HPβCD and the solubility-permeability interplay [J].
Beig, Avital ;
Agbaria, Riad ;
Dahan, Arik .
EUROPEAN JOURNAL OF PHARMACEUTICAL SCIENCES, 2015, 77 :73-78
[6]   The interaction of nifedipine with selected cyclodextrins and the subsequent solubility-permeability trade-off [J].
Beig, Avital ;
Miller, Jonathan M. ;
Dahan, Arik .
EUROPEAN JOURNAL OF PHARMACEUTICS AND BIOPHARMACEUTICS, 2013, 85 (03) :1293-1299
[7]   Oral Delivery of Lipophilic Drugs: The Tradeoff between Solubility Increase and Permeability Decrease When Using Cyclodextrin-Based Formulations [J].
Beig, Avital ;
Agbaria, Riad ;
Dahan, Arik .
PLOS ONE, 2013, 8 (07)
[8]   Accounting for the solubility-permeability interplay in oral formulation development for poor water solubility drugs: The effect of PEG-400 on carbamazepine absorption [J].
Beig, Avital ;
Miller, Jonathan M. ;
Dahan, Arik .
EUROPEAN JOURNAL OF PHARMACEUTICS AND BIOPHARMACEUTICS, 2012, 81 (02) :386-391
[9]   BDDCS Applied to Over 900 Drugs [J].
Benet, Leslie Z. ;
Broccatelli, Fabio ;
Oprea, Tudor I. .
AAPS JOURNAL, 2011, 13 (04) :519-547
[10]   COMPARED EFFECTS OF SYNTHETIC AND NATURAL BILE-ACID SURFACTANTS ON XENOBIOTIC ABSORPTION .1. STUDIES WITH POLYSORBATE AND TAUROCHOLATE IN RAT COLON [J].
BERMEJO, MV ;
PEREZVARONA, AT ;
SEGURABONO, MJ ;
MARTINVILLODRE, A ;
PLADELFINA, JM ;
GARRIGUES, TM .
INTERNATIONAL JOURNAL OF PHARMACEUTICS, 1991, 69 (03) :221-231