Solubilization of Therapeutic Agents in Micellar Nanomedicines

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• 作者：Lela Vukovi? ; Antonett Madriaga ; Antonina Kuzmis ; Amrita Banerjee ; Alan Tang ; Kevin Tao ; Neil Shah ; Petr Král ; Hayat Onyuksel
• 刊名：Langmuir
• 出版年：2013
• 出版时间：December 23, 2013
• 年：2013
• 卷：29
• 期：51
• 页码：15747-15754
• 全文大小：528K
• ISSN：1520-5827

文摘

We use atomistic molecular dynamics simulations to reveal the binding mechanisms of therapeutic agents in PEG-ylated micellar nanocarriers (SSM). In our experiments, SSM in buffer solutions can solubilize either 鈮?1 small bexarotene molecules or 鈮? (2 in low ionic strength buffer) human vasoactive intestinal peptide (VIP) molecules. Free energy calculations reveal that molecules of the poorly water-soluble drug bexarotene can reside at the micellar ionic interface of the PEG corona, with their polar ends pointing out. Alternatively, they can reside in the alkane core center, where several bexarotene molecules can self-stabilize by forming a cluster held together by a network of hydrogen bonds. We also show that highly charged molecules, such as VIP, can be stabilized at the SSM ionic interface by Coulombic coupling between their positively charged residues and the negatively charged phosphate headgroups of the lipids. The obtained results illustrate that atomistic simulations can reveal drug solubilization character in nanocarriers and be used in efficient optimization of novel nanomedicines.