Effects of vehicle on diclofenac sodium permeation from new topical formulations: in vitro and in vivo studies
Academic Article
Publication Date:
2009
Short description:
Effects of vehicle on diclofenac sodium permeation from new topical formulations: in vitro and in vivo studies / Vanna, S., Peana, A.T., Moretti, M.D.L.. - In: CURRENT DRUG DELIVERY. - ISSN 1567-2018. - 6:1(2009), pp. 93-100. [10.2174/156720109787048311]
abstract:
In this study the effect of vehicle on in vitro diffusion of diclofenac sodium (DS) from new different formulations
such as Carbopol gel (A), Sodium lauryl sulphate cream (B) and Carbopol cream (C) was evaluated with Franz diffusion
cells using hydrophilic and hydrophobic synthetic membranes. The commercial formulation Voltaren® Emulgel
was used as reference.
Furthermore, the in vivo efficacy of topical formulations was studied in the carrageenan-induced edema and hyperalgesia,
whereas the antinociceptive effect was evaluated on thermal pain threshold in rat paw.
The flux of DS across hydrophilic membranes showed this rank order: Control C > A B. On the other hand, the diffusion
rate of DS across hydrophobic membranes resulted in the following order: Control > B > A C; this suggested a
lower interaction between the vehicles and these membranes.
The in vivo results indicated that the prepared formulations failed in the inflammatory tests to reduce the development of
edema.
Nevertheless, treatment with B formulation inhibited the development of acute hyperalgesia induced by carrageenan, and
elicited a significant increase in paw withdrawal latencies whereas other formulations were ineffective.
The results obtained in this study suggest that Sodium lauryl sulphate cream might be useful in local pain conditions and
may be an effective alternative to the presently used systemic routes.
such as Carbopol gel (A), Sodium lauryl sulphate cream (B) and Carbopol cream (C) was evaluated with Franz diffusion
cells using hydrophilic and hydrophobic synthetic membranes. The commercial formulation Voltaren® Emulgel
was used as reference.
Furthermore, the in vivo efficacy of topical formulations was studied in the carrageenan-induced edema and hyperalgesia,
whereas the antinociceptive effect was evaluated on thermal pain threshold in rat paw.
The flux of DS across hydrophilic membranes showed this rank order: Control C > A B. On the other hand, the diffusion
rate of DS across hydrophobic membranes resulted in the following order: Control > B > A C; this suggested a
lower interaction between the vehicles and these membranes.
The in vivo results indicated that the prepared formulations failed in the inflammatory tests to reduce the development of
edema.
Nevertheless, treatment with B formulation inhibited the development of acute hyperalgesia induced by carrageenan, and
elicited a significant increase in paw withdrawal latencies whereas other formulations were ineffective.
The results obtained in this study suggest that Sodium lauryl sulphate cream might be useful in local pain conditions and
may be an effective alternative to the presently used systemic routes.
Iris type:
1.1 Articolo in rivista
Keywords:
Diclofenac sodium; in vitro diffusion; in vivo studies
List of contributors:
Vanna, Sanna; Peana, ALESSANDRA T.; Moretti, Mario Domenico Luigi
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