Mahato Ram I, Narang Ajit S, Thoma Laura, Miller Duane D
Department of Pharmaceutical Sciences, University of Tennessee Health Science Center, Memphis, Tennessee 38163, USA.
Crit Rev Ther Drug Carrier Syst. 2003;20(2-3):153-214. doi: 10.1615/critrevtherdrugcarriersyst.v20.i23.30.
Most peptide and protein drugs are currently used as parenteral formulations because of their poor oral bioavailability. Development of an effective oral delivery system for these macromolecular drugs requires a thorough understanding of their physicochemical properties, such as molecular weight, hydrophobicity, ionization constants, and pH stability, as well as biological barriers that restrict protein and peptide absorption from the gastrointestinal (GI) tract, including pH variability, enzymatic degradation, and membrane efflux. Various strategies currently under investigation include amino acid backbone modifications, formulation approaches, chemical conjugation of hydrophobic or targeting ligand, and use of enzyme inhibitors, mucoadhesive polymers, and absorption enhancers. However, there is only limited success because of the hostile environment of the GI tract--e.g., strong pH extremes and abundant presence of potent luminal enzymes. This review focuses on the challenges posed by the GI system and how different pharmaceutical approaches can be used to make oral delivery of protein and peptide drugs more feasible. The roles of P-glycoprotein and CYP3A4 in controlling the extent of intestinal absorption and metabolism will also be discussed.
由于大多数肽类和蛋白质药物口服生物利用度较差,目前它们大多以肠胃外制剂的形式使用。开发针对这些大分子药物的有效口服给药系统需要深入了解其物理化学性质,如分子量、疏水性、电离常数和pH稳定性,以及限制蛋白质和肽从胃肠道吸收的生物屏障,包括pH变化、酶降解和膜外排。目前正在研究的各种策略包括氨基酸主链修饰、制剂方法、疏水或靶向配体的化学偶联,以及使用酶抑制剂、粘膜粘附聚合物和吸收促进剂。然而,由于胃肠道的恶劣环境,如极端的pH值和大量强效腔内酶的存在,成功案例有限。本综述重点关注胃肠道系统带来的挑战,以及如何采用不同的制药方法使蛋白质和肽类药物的口服给药更可行。还将讨论P-糖蛋白和CYP3A4在控制肠道吸收和代谢程度方面的作用。
Crit Rev Ther Drug Carrier Syst. 2003
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