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Background: Corneal neovascularization is a sight-threatening disease. It can be treated using antiangiogenic and anti-inflammatory compounds. Therefore, atorvastatin (ATV) constitutes a suitable candidate to be administered topically. To attain suitable efficacy, ATV can be encapsulated into custom-developed nanocarriers such as peptide amphiphiles. Methods: Three peptide amphiphiles bearing one, two or four C16-alkyl groups (mC16-Tat47-57, dC16-Tat47-57 and qC16-Tat47-57) were synthesized, characterized and loaded with ATV. Drug release and ocular tolerance were assessed as well as anti-inflammatory and antiangiogenic properties. Results: ATV-qC16-Tat47-57 showed higher encapsulation efficiency than mC16-Tat47-57 and dC16-Tat47-57 and more defined nanostructures. ATV-qC16-Tat47-57 showed ATV prolonged release with suitable ocular tolerance. Moreover, ATV-qC16-Tat47-57 was antiangiogenic and prevented ocular inflammation. Conclusion: ATV-qC16-Tat47-57 constitutes a promising topical medication against corneal neovascularization.
Drug Liberation, Drug delivery, Ocular inflammation, Atorvastatin, Humans, Corneal Neovascularization, Angiogenesis, Peptide amphiphiles, http://metadata.un.org/sdg/3, Eye, Peptides, Ensure healthy lives and promote well-being for all at all ages
Drug Liberation, Drug delivery, Ocular inflammation, Atorvastatin, Humans, Corneal Neovascularization, Angiogenesis, Peptide amphiphiles, http://metadata.un.org/sdg/3, Eye, Peptides, Ensure healthy lives and promote well-being for all at all ages
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