Table 1. Literature data on medicated foams vs. other cutaneous pharmaceutical forms.
| Drug | Set-up | Main Findings | Year | Refs. |
|---|---|---|---|---|
| In vitro | ||||
| Clindamycin | Human skin; flow-through diffusion cells vs. gel | Greater accumulation after 24 h and earlier onset than clindamycin gel. | 2005 | [7] |
| Clobetasol propionate |
Human skin; flow-through diffusion cells vs. cream, emollient cream, lotion, and solution | A faster initial permeation of clobetasol compared with the other vehicles. In the first 14 h, foam delivered a similar amount of drug (J and AUC) compared with the emollient cream and a greater amount of drug compared with the solution, cream, and lotion. The foam vehicle delivered more clobetasol than the other formulations. | 2005 | [7] |
| Clobetasol propionate |
Different anatomic region of human skin vs. foam, cream, and emollient cream | Foam needs the least time to overcome anatomic region variations (= thickness), whereas cream and ointment take a longer time for the onset of delivery. | 2005 | [7] |
| Ketoconazole | Silastic membranes; static Franz cells | Penetration 11-fold higher vs. cream. | 2005 | [7] |
| Metronidazole | In vitro skin penetration study; excised human skin; a flow-through diffusion cell | The total cutaneous penetration of metronidazole was two- to three-fold higher than the reference cream. | 2006 | [8] |
| Vitamin E acetate |
In vitro silicone membrane penetration study; in vitro skin tape stripping |
The increase in Pluronic surfactant concentration after application modified the lipid nanoparticles to enable drug release and penetration into skin. | 2009 | [9] |
| Benzoyl peroxide | In vitro silicone membrane penetration study | Benzoyl peroxide loaded in nanoparticles was chemically stable over a 7 d period. Foams allowed to obtain a comparable flux to commercial gels and creams, but at much lower concentration. | 2010 | [10] |
| Minoxidil | In vitro silicone membrane penetration study | Foam delivered significantly more drugs across the membrane than the saturated aqueous solution. The cumulative permeant amount of drug depends on the surfactant concentration in the foam. | 2010 | [11] |
| Calcipotriene + betamethasone | Raman imaging | After propellant evaporation, a supersaturated environment was created, where drug crystals were absent for at least 26 h. | 2016 | [12] |
| Thiocolchicoside | Skin; Saarbruecken penetration model-based cells | At each incubation time, significant higher amounts of drug were detected for the foam formulation. | 2008 | [13] |
| Cholecalciferol + salicylic acid | Pig-ear test for irritancy potential evaluation | Incorporation of two incompatible drugs. | 2017 | [14] |
| In vivo | ||||
| Minoxidil | Caucasian male volunteers aged between 22 and 29 years. Every 10 d, 0.007±0.002 g foam was applied to the chest and the occipital region of the scalp | Hair follicles contribute to the penetration of minoxidil into the blood circulation since faster absorption of minoxidil was detected when the hair follicle orifices were open. | 2010 | [15] |
| Betamethasone valerate | A Phase II, randomised, single-centre, blinded, right-left comparison within 30 patients with mild-to-moderate psoriasis | After 3 wk, statistical significant improvement from baseline in thickness, redness, scaling, itch and global score. | 2006 | [8] |
| Tarazotene | Phase I study | Reduced systemic levels of tazarotenic acid in comparison to the marketed gel. | 2013 | [16] |
| Azelaic acid | A Phase 3 randomized, double-blind, vehicle-controlled, parallel-group, multicenter study with participants with moderate to severe papulopustular rosacea | Azelaic acid foam at 15% resulted efficient and safe in patients with papulopustular rosacea. | 2015 | [17] |
| Azelaic acid | Eight dogs with nonseasonal mild/moderate canine atopic dermatitis were treated twice weekly with either a commercial foam or a foam/mousse containing components from plant extracts, for 14 d. After a wash-out period of 14 d received the other foam in a randomized blinded study | A significant improvement in both skin lesions and pruritus was noted for both treatment groups. This method of product delivery is easy to use for owners, improving compliance in practice. | 2018 | [18] |
| Econazole nitrate | Two randomized, double-blind, parallel-group, vehicle-controlled, multicenter studies enrolled males and females ≥12 y old with a clinical diagnosis of interdigital tinea pedis and baseline fungal culture positive for a dermatophyte. Subjects applied 1% econazole nitrate foam (n=246) or foam vehicle (n=249) once daily for 4 wk | The drug-loaded foam exhibited superiority over foam vehicle with a high mycologic cure rate for all pathogens evaluated. Econazole nitrate foam 1% was safe and well tolerated with a safety profile comparable with the foam vehicle. | 2014 | [19] |
| Tazarotene | Two randomized, double-blind, vehicle-controlled, parallel-group studies were randomly treated with either0.1% tazarotene foam or vehicle foam once daily for 12 wk | Tazarotene foam significantly reduced the number and severity of acne lesions after 12 wk and had a safe and acceptable tolerability profile. | 2013 | [20] |