Review of Clinical Evidence over 10 Years on Prevention and Treatment of a Film-Forming Medical Device Containing Photolyase in the Management of Field Cancerization in Actinic Keratosis

The product is a film-forming medical device that contains organic and inorganic UVB and UVA sun filters together with a DNA repair enzyme photolyase entrapped in liposomes.

Eryfotona AK-NMSC acts by forming a film on the skin, thus protecting from both UVA and UVB radiation. The content of UVA and UVB filters and the vehicle used confer to the product a broad-spectrum protection and a very high SPF (100+). Eryfotona AK-NMSC also contains the DNA repair enzyme photolyase. This light-activated flavoenzyme derived from the algae Anacystis nidulans is unique in that it utilizes the energy from visible blue light (a process called photoreactivation) to revert CPDs and pyrimidine–pyrimidone (6–4) photoproducts. Similar to the DNA repair enzyme T4 endonuclease, photolyase has been entrapped in pH-sensitive multilamellar liposomes. The liposome encapsulation of DNA repair enzymes such as T4 endonuclease V and photolyase represents a new delivery system approach that shuttles these biologically active DNA repair enzymes into the epidermis and inside the keratinocytes [43‐46]. Topical photolyase restores CPDs faster and more effectively than topical endonuclease [46]. This difference can be attributed to the fact that topical application of photolyase and photoreactivation transiently provides an additional repair system to human cells. UV filters together with photolyase mechanisms contribute to the strengthening of DNA repair and protect DNA from further UV-mediated damage.

Eryfotona AK-NMSC also contains several ingredients with emollient and skin-conditioning functions, which act on dryness, scaling, and erythema associated with chronically UV exposed AK skin.

This article is based on previously conducted studies and does not contain any studies with human participants or animals performed by any of the authors.

Since the launch of Eryfotona in 2008, 11 clinical studies have been conducted assessing the beneficial effect of Eryfotona AK-NMSC on the treatment and prevention of AK lesions and on improvement of the field of cancerization in patients with mild to moderate AK. Taking together the results of the 11 clinical studies involving 228 subjects, there is enough evidence to indicate that the use of Eryfotona AK-NMSC is beneficial in AK patients [2] even though the majority of these studies were open-label and involved small numbers of patients. A summary of these studies is provided in Supplementary Table 2.

Several researchers have presented the outcomes of studies undertaken during the last 10 years in different congresses and in peer-reviewed journals. In this review, we focused on the effect of Eryfotona AK-NMSC at the cellular, histological, and clinical level. Treatment with Eryfotona AK-NMSC applied either alone or in combination with other therapies has been associated with a reduction in the number of lesions, improvement in macroscopic and microscopic characteristics of lesions, and a reduction in appearance of new lesions.

Between 2013 and 2015, the first studies were published using different diagnostic techniques in order to demonstrate the benefits of Eryfotona AK-NMSC as a single treatment for patients with AK lesions. Puviani et al. [47] published a series of six case studies showing that Eryfotona AK-NMSC for periods of 4 weeks to 2 months is efficient in the treatment of AK lesions and of cancerization field, without side effects. In 2015, the same authors published the outcomes of a pilot, prospective, open-label study with 11 AK patients [48] showing that Eryfotona AK-NMSC treatment for 3 months led to a 75% reduction in the AK lesion area which was both statistically significant and clinically relevant compared to baseline. The product was well tolerated.

These data are consistent with the results reported by Laino et al. [3] according to which treatment with Eryfotona AK-NMSC for 9 months was effective in reducing the hyperthermic halo around AK lesions in all the 27 patients who completed the study, while in five of them the hyperthermic halo disappeared completely. Hyperthermic halo is defined as the area surrounding a tumor lesion that can be detected by active telethermography and can represent the visible expression of the cancerization field [3].

At the same time, studies were carried out to identify which immunological or histochemical markers can reflect the improvement in the field of cancerization after a short treatment period (from 2 to 3 months).

In 2013, Puig-Butillé et al. published a study to evaluate the molecular effects of Eryfotona AK-NMSC on the precancerous field in seven AK patients through histopathological and molecular evaluation [49]. Patients were classified into fast and partial responders and it was shown that there were expression level differences for the CPI-17 gene confirmed by RT-PCR between fast and partial responders both before and after treatment. The authors concluded that 1-month treatment with Eryfotona AK-NMSC improved the field of cancerization and restored normal phenotype in at least a subset of samples, through CPI-17 upregulation.

Following this line of research, Puig et al. published a clinical study evaluating the effects of topical Eryfotona AK-NMSC application on the cancerization field in patients with AK [31]. Thirteen AK patients were instructed to use either Eryfotona AK-NMSC or a comparator containing the same organic and inorganic UVB-UVA filters (SPF 100+) without photolyase. Assessments included clinical, dermoscopic, and reflectance confocal microscopy (RCM) assessments, as well as skin biopsies, before and after the 4-week treatment. The authors reported a clinically evident improvement in erythema and scaling with Eryfotona AK-NMSC. Moreover, RCM assessment showed a marked reduction in scaling, detached corneocytes and polygonal nucleated cells in the stratum corneum, an improvement of the atypical honeycomb pattern, and fewer round nucleated cells at the spinous granulous layer with Eryfotona AK-NMSC while no improvement was noted with the comparator product. Histopathological findings indicated that after a 4-week treatment, 50% of patients showed complete histological clearance. In other words, in these patients, the epidermal morphology was no longer consistent with a diagnosis of AK. These findings were supported with data from immunohistochemistry obtained from biopsies at baseline vs end of the 4-week treatment showing decreased p21 expression (a pro-apoptotic marker) in suprabasal layers and a trend for reduction in proliferating cell nuclear antigen (PCNA, a marker for proliferation) in the basal layer. The authors suggested that longer follow-up studies with biopsy assessments at 3 or 12 months may allow evaluation of the impact of Eryfotona AK-NMSC on p53 expression.

In agreement with these observations are the results of another clinical study conducted in 2014 by Rstom et al. [50] showing that Eryfotona AK-NMSC contributes to a dermoscopic and histological improvement of AK lesions. This study reported that after Eryfotona AK-NMSC application for 4 months, grade I lesions presented less desquamation and an improvement in epidermal pattern.

The demonstrated evidence of Eryfotona AK-NMSC as a unique treatment in cases of low number of AK lesions has led to research into whether Eryfotona AK-NMSC can also act on more severe cases of AK, in which patients present many AK lesions either due to genetic background or to a state of immunosuppression due to advanced age or treatment for other conditions.

Giustini et al., in 2014, reported data from a retrospective analysis of the use of Eryfotona AK-NMSC in eight patients diagnosed with xeroderma pigmentosum who as a result of a genetic defect of the DNA repair system have increased rates of AK and other premalignant and malignant skin lesions. Treatment with Eryfotona AK-NMSC was associated with a 65% reduction in the appearance of new AK lesions and with 56% and 100% reduction in the incidence of new BCC and SCC lesions [51].

Along the same lines, Navarrete-Dechent and Molgó [52] undertook a prospective, single-arm, case series to evaluate the effect of Eryfotona AK-NMSC applied twice daily for 3 months on nine patients with field cancerization and multiple AKs. The study showed an absolute reduction of 76.6% in the number of AK lesions, with the mean number of lesions reduced from 13.4 to 3.1 without reported adverse events.

Three studies compared the effect of Eryfotona AK-NMSC to very high protection sunscreens (SPF 50+). The outcomes of the studies show that treatment with Eryfotona AK-NMSC leads to a reduction of the number of new lesions, as well as to a clinical, dermoscopic, and histological improvement of existing lesions.

Moscarella et al. evaluated the effects of a 6-month treatment with Eryfotona AK-NMSC vs sunscreen SPF50+ in a prospective, randomized, parallel, double-blind, pilot study [53]. Fifty patients with at least four AK lesions at the same anatomical photo-exposed area were enrolled and 36 patients completed the study. Patients were instructed to use either product twice daily and were not receiving any other treatment for AK during the study. Clinical evaluation, dermoscopy, and RCM were used to evaluate AK lesions at baseline, after 4 weeks, 3 months, and 6 months of treatment. After 6 months of treatment, there was a significant reduction in the mean number of AK lesions vs baseline in the Eryfotona and sunscreen group; both groups also improved Baseline Severity Index (BSI) and Total Clinical Score (TCS) in the subgroup representing mild AK (less than 10 lesions in target area at baseline). The Eryfotona AK-NMSC arm showed a significant decrease in the number of AK lesions in the target area and a significant improvement of clinical parameters such as BSI and TCS including mean changes of scaling, erythema, pigmentation, and follicular plugs. Importantly, Eryfotona AK-NMSC was more effective than sunscreen in preventing the appearance of new lesions. This effect was statistically significant 3 months after initiating the treatment and persisted as a strong trend until the end of the study (6 months). In the subgroup of patients with less than 10 lesions, only 14% of the Eryfotona AK-NMSC-treated patients presented new lesions at the end of the study compared to 54% of the patients using sunscreen [53].

The results in patients with mild AK confirm that Eryfotona AK-NMSC is a relevant therapy in the management of the cancerization field and offers superior benefits compared to the use of sunscreen alone.

In a prospective, parallel, assessor-blinded, two-arm study conducted by Eibenschutz et al., the effect of Eryfotona AK-NMSC vs sunscreen (SPF 50+) was evaluated in 30 AK patients after a successful PDT [54]. Participants were randomly assigned to either Eryfotona AK-NMSC or sunscreen group. Both groups had comparable lesion counts at baseline. Participants were instructed to apply either product in a similar fashion, twice daily for 9 consecutive months. At the end of the 9-month period, the appearance of new lesions in the previously PDT-treated area and the need for another session of PDT or similar therapy was evaluated. A progressive increase in number of AK lesions was observed in the sunscreen group (mean lesion number of 3.6 at the end of the study in comparison to 0.6 just after the PDT session). In comparison, in the Eryfotona AK-NMSC group a significant reduction of AK lesions and lack of new lesions were observed (mean lesion number of 1.0 at the end of the study in comparison to 2.0 after the PDT session). In the sunscreen treated group, 15 subjects (86%) presented new AK lesions during the study either in PDT-treated areas or in new areas. From these, 10 patients (66%) needed a new PDT session or a field-targeted treatment, while no patients in the Eryfotona AK-NMSC group needed a new PDT session or another field-targeting treatment.

Overall, it can be concluded that the beneficial effect of Eryfotona AK-NMSC in comparison to very high protection sunscreen is evident in terms of reduction in the number of new and existing lesions and no need for additional PDT or another field-targeted treatment.

Eryfotona AK-NMSC is also effective in reducing the number of existing and new lesions when applied in combination with cryotherapy.

An observational study conducted by Vaño-Galván et al. evaluated the effect of Eryfotona AK-NMSC in conjunction with cryotherapy on AKs and cancerization field in 41 patients with at least four clinical AK lesions [55]. The participants applied Eryfotona AK-NMSC twice daily for 6 months, starting on the day following cryotherapy. At the end of the 6-month period, the number of AK lesions decreased in comparison to baseline (a mean number of 9.56 lesions was observed at baseline and 1.51 at 6 months). The effect was better manifested in thin AK lesions (grade I–II lesions as per investigator criterion).

On the other hand, the mean number of new lesions was 0.27 at the end of the first month and 0.76 at the end of the sixth month, suggesting a possible protective effect on the appearance of new lesions. It has previously been shown that cryotherapy is effective only in 68% of AK cases. Additionally, 96% of subjects treated with cryotherapy present new lesions 1 year after completion of treatment [55]. The results of the Vaño-Galván et al. study suggest that Eryfotona AK-NMSC could have a beneficial effect on the cancerization field by reducing the incidence of new lesions following cryotherapy. Although an important limitation of this study is the lack of a control group, these results are of interest as Eryfotona AK-NMSC could potentially represent a good therapeutic strategy allowing more time between cryotherapy sessions in patients with AK.