Abstract

In recent years, advanced nanohybrid materials processed as pharmaceuticals have proved to be very advantageous. Triptans, such as the commercially available intranasal sumatriptan (SMT), are drugs employed in the treatment of painful migraine symptoms. However, SMT effectiveness by the intranasal route is limited by its high hydrophilicity and poor mucoadhesion. Therefore, we designed hybrid nanoemulsions (NE) composed of copaiba oil as the organic component plus biopolymers (xanthan, pectin, alginate) solubilized in the continuous aqueous phase, aiming at the intranasal release of SMT (2% w/v). Firstly, drug-biopolymer complexes were optimized in order to decrease the hydrophilicity of SMT. The resultant complexes were further encapsulated in copaiba oil-based nanoparticles, forming NE formulations. Characterization by FTIR-ATR, DSC, and TEM techniques exposed details of the molecular arrangement of the hybrid systems. Long-term stability of the hybrid NE at 25°C was confirmed over a year, regarding size (~ 120 nm), polydispersity (~ 0.2), zeta potential (~ −25 mV), and nanoparticle concentration (~ 2.1014 particles/mL). SMT encapsulation efficiency in the formulations ranged between 41–69%, extending the in vitro release time of SMT from 5 h (free drug) to more than 24 h. The alginate-based NE was selected as the most desirable system and its in vivo nanotoxicity was evaluated in a zebrafish model. Hybrid NE treatment did not affect spontaneous movement or induce morphological changes in zebrafish larvae, and there was no evidence of mortality or cardiotoxicity after 48 h of treatment. With these results, we propose alginate-based nanoemulsions as a potential treatment for migraine pain.

Highlights

  • Migraines are one of the top 10 causes of work disability in the world (Natoli et al, 2010; Vos et al, 2015)

  • The parameters analyzed for a year (25◦C) were: size, polydispersity index (PDI), TABLE 1 | Sumatriptan (2%) encapsulation efficiency (%EE) in NE and in the hybrid biopolymer-NE formulations

  • This work aimed at the development of hybrid nanoemulsions composed of copaiba oil and biopolymers for the loading of sumatriptan (2%) for intranasal administration

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Summary

Introduction

Migraines are one of the top 10 causes of work disability in the world (Natoli et al, 2010; Vos et al, 2015). It is a painful and limiting disease with a prevalence above 20% (Yeh et al, 2018), characterized by periodic headache outbreaks, often associated with gastric problems and photo/phonophobia. In the late 1980s, some serotonin agonists, known as triptans, were developed for the treatment of migraine. Intranasal sumatriptan (SMT) is the gold standard treatment for severe migraines (Muzzi et al, 2020). There are no effective drugs available for treating migraines

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