Methotrexate
(MTX) is one of the first-line treatments for moderate
to severe psoriasis, while the side effects caused by injection and
oral administration of MTX greatly restrict its clinical application.
Transdermal drug delivery offers a desirable alternative to the conventional
approaches, but the performances of the currently available skin penetration
enhancement techniques are not so satisfactory. To address these limitations,
we developed a dissolving microneedle (MN) patch made of hyaluronic
acid (HA) with excellent water solubility, biocompatibility, biodegradability,
and mechanical properties. The amount of MTX encapsulated in the needles
of the patch could be controlled during the fabrication process for
precise dosage. Interestingly, the MTX-loaded MNs successfully penetrated
imiquimod (IMQ)-induced thickened epidermis in mice and delivered
the drug intralesionally. Meanwhile, fast dissolution of HA endowed
the MNs with operability for patients. We found that the MTX-loaded
MNs not only showed well-maintained inhibitory effect in vitro but
also alleviated the psoriasis-like skin inflammation in mice. Moreover,
the MTX-loaded MNs were significantly more efficacious than taking
the same dose of drug orally. Consequently, a higher oral dose of
MTX was required for a comparable amelioration, which in turn increased
its systemic toxicity. Taken together, the proposed MTX-loaded dissolving
MN patch strategy provides a new opportunity for efficient and safe
treatment of psoriasis.
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