Strategic development of aceclofenac loaded organosomes for topical application: An explorative ex-vivo and in-vivo investigation for arthritis.

Int J Pharm

University Institute of Pharmaceutical Sciences, UGC-centre of Advanced Studies, Panjab University, Chandigarh 160014, India. Electronic address:

Published: December 2024

AI Article Synopsis

  • The study focuses on creating aceclofenac-encapsulated organosomes (OS) designed to treat arthritis using a unique combination of phospholipids and organic solvents.
  • The OS formulation showed promising characteristics such as a small size, high drug entrapment efficiency, and improved drug permeability compared to a marketed product, leading to better penetration in skin layers.
  • Results from various arthritis models demonstrated that the OS significantly reduced inflammation markers and was more effective in alleviating arthritis symptoms than the marketed product.

Article Abstract

Present study intends to develop aceclofenac-encapsulated organosomes (OS), which consist of phospholipids coupled with a combination of organic solvents, for the management of arthritis. The formulation was characterized and tested for efficacy using formalin-induced hyperalgesia, air pouch, and CFA-induced arthritic rat models. OS system exhibited spherical dimension, nanometric size with low PDI (278.3 ± 12.21 nm; 0.145), zeta potential (-24.56 ± 7.53 mV), drug entrapment (85.62 ± 7.2 %) and vesicles count (4.2x104 mm). The gelled OS formulation demonstrated increased drug permeability and accumulation rate (51.77 ± 7.1 % and 396.19 ± 59.21 µg/cm) compared to the MKT product (102.93 ± 13.78 µg/cm and 16.14 ± 4.3 %). Dermatokinetic assessments exhibited significantly higher drug levels in dermal layers compared to MKT product (p < 0.001), and CLSM studies further supported the OS system's deeper penetration. The results of arthritic index significantly better (9 times) in the OS-treated group than the MKT product. OS system treatment significantly reduced biochemicals and cytokines levels, such as CRP, ESR, TLC, lymphocytes, TNF-α, IL-6, and IL-1β to levels of the control group (p < 0.001). Pseudoplastic behaviour of the developed product was indicated by the rheological results, and it also demonstrated biocompatibility through skin compliance studies. Based on the current findings, it appears that OS may be a better choice for managing arthritis and related inflammations.

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Source
http://dx.doi.org/10.1016/j.ijpharm.2024.124762DOI Listing

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