AI Article Synopsis

  • The study investigates the effectiveness of intranasal drug delivery for targeting the brain, focusing on two absorption pathways: trans-neuronal for quick effects and para-neuronal for delayed effects.
  • The researchers used lidocaine to block the olfactory nerve's action potential and tested a radiolabeled anti-Parkinson drug, ropinirole, to compare its absorption in challenged rabbits and rats.
  • Results indicated a significant increase in drug concentration in the brain using both pathways, highlighting the importance of formulation strategies to optimize drug delivery for treating CNS disorders.

Article Abstract

The effectiveness of intranasal drug delivery for brain targeting has emerged as a hope of remedy for various CNS disorders. The nose to brain absorption of therapeutic molecules claims two effective pathways, which include trans-neuronal for immediate action and para-neuronal for delayed action. To evaluate the contribution of both the pathways in absorption of therapeutic molecules and nanocarriers, lidocaine, a nerve-blocking agent, was used to impair the action potential of olfactory nerve. An anti-Parkinson drug ropinirole was covalently complexes with (99m)Tc in presence of SnCl2 using in-house developed reduction technology. The radiolabeled formulations were administered intranasally in lidocaine challenged rabbit and rat. The qualitative and quantitative outcomes of neural and non-neural pathways were estimated using gamma scintigraphy and UHPLC-MS/MS, respectively. The results showed a significant (p ≤ 0.005) increase in radioactivity counts and drug concentration in the brain of rabbit and rat compared to the animal groups challenged with lidocaine. This concludes the significant contribution (p ≤ 0.005) of trans-neuronal and para-neuronal pathway in nose to brain drug delivery. Therefore, results proved that it is an art of a formulator scientist to make the drug carriers to exploit the choice of absorption pathway for their instant and extent of action.

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Source
http://dx.doi.org/10.3109/10717544.2014.923064DOI Listing

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