Institute for Drug Research, School of Pharmacy, Faculty of Medicine , The Hebrew University of Jerusalem , P.O. Box 12065, Jerusalem 91120 , Israel.
Institute for Advanced Study and Center of Integrated Protein Science, Department Chemie , Technische Universität München , Lichtenbergstrasse 4 , 85748 Garching , Germany.
Mol Pharm. 2018 Aug 6;15(8):3468-3477. doi: 10.1021/acs.molpharmaceut.8b00466. Epub 2018 Jul 25.
Hydrophilic peptides constitute most of the active peptides. They mostly permeate via tight junctions (paracellular pathway) in the intestine. This permeability mechanism restricts the magnitude of their oral absorption and bioavailability. We hypothesized that concealing the hydrophilic residues of the peptide using the lipophilic prodrug charge masking approach (LPCM) can improve the bioavailability of hydrophilic peptides. To test this hypothesis, a cyclic N-methylated hexapeptide containing Arg-Gly-Asp (RGD) and its prodrug derivatives, masking the Arg and Asp charged side chains, were synthesized. The library was evaluated for intestinal permeability in vitro using the Caco-2 model. Further investigation of metabolic stability ex vivo models in rat plasma, brush border membrane vesicles (BBMVs), and isolated CYP3A4 microsomes and pharmacokinetic studies was performed on a selected peptide and its prodrug (peptide 12). The parent drug analogues were found to have a low permeability rate in vitro, corresponding to atenolol, a marker for paracellular permeability. Moreover, palmitoyl carnitine increased the P of peptide 12 by 4-fold, indicating paracellular permeability. The P of the prodrug derivatives was much higher than that of their parent peptides. For instance, the P of the prodrug 12P was 20-fold higher than the P of peptide 12 in the apical to basolateral (AB) direction. Whereas the permeability in the opposite direction (BA of the Caco-2 model) was significantly faster than the P AB, indicating the involvement of an efflux system. These results were corroborated when verapamil, a P-gp inhibitor, was added to the Caco-2 model and increased the P AB of prodrug 12P by 3-fold. The prodrug 12P was stable in the BBMVs environment, yet degraded quickly (less than 5 min) in the plasma into the parent peptide 12. Pharmacokinetic studies in rats showed an increase in the bioavailability of peptide 12 > 70-fold (from 0.58 ± 0.11% to 43.8 ± 14.9%) after applying the LPCM method to peptide 12 and converting it to the prodrug 12P. To conclude, the LPCM approach converted the absorption mechanism of the polar peptides from a paracellular to transcellular pathway that tremendously affects their oral bioavailability. The LPCM method provides a solution for the poor bioavailability of RGD cyclohexapeptides and paves the way for other active hydrophilic and charged peptides with poor oral bioavailability.
亲水肽构成了大多数活性肽。它们主要通过肠道中的紧密连接(细胞旁途径)渗透。这种渗透机制限制了它们口服吸收和生物利用度的程度。我们假设,使用亲脂性前药电荷掩蔽方法(LPCM)掩盖肽的亲水残基可以提高亲水肽的生物利用度。为了验证这一假设,我们合成了一种含有精氨酸-甘氨酸-天冬氨酸(RGD)的环状 N-甲基化六肽及其掩蔽精氨酸和天冬氨酸带电侧链的前药衍生物。该文库使用 Caco-2 模型在体外评估了肠道通透性。进一步在大鼠血浆、刷状缘膜囊泡(BBMV)和分离的 CYP3A4 微粒体以及选定的肽及其前药(肽 12)的体外代谢稳定性模型中进行了研究。结果发现,亲本药物类似物在体外的通透性很低,与作为细胞旁通透性标志物的阿替洛尔相当。此外,肉毒碱增加了肽 12 的 P 值 4 倍,表明存在细胞旁通透性。前药衍生物的 P 值远高于其母体肽。例如,前药 12P 的 P 值比其母体肽在顶侧到基底侧(AB)方向上高 20 倍。而在相反方向(Caco-2 模型的 BA)的通透性明显快于 P AB,表明存在外排系统的参与。当在 Caco-2 模型中加入 P-糖蛋白抑制剂维拉帕米时,这些结果得到了证实,前药 12P 的 P AB增加了 3 倍。前药 12P 在 BBMV 环境中稳定,但在血浆中迅速降解(不到 5 分钟)为母体肽 12。在大鼠中的药代动力学研究表明,应用 LPCM 方法将肽 12 转化为前药 12P 后,其生物利用度增加了超过 70 倍(从 0.58±0.11%增加到 43.8±14.9%)。总之,LPCM 方法将极性肽的吸收机制从细胞旁途径转变为细胞内途径,极大地影响了它们的口服生物利用度。LPCM 方法为 RGD 环六肽的低生物利用度提供了一种解决方案,并为其他具有低口服生物利用度的亲水性和带电活性肽铺平了道路。
