Adapalene Gel 0.1% Versus Placebo as Prophylaxis for Anti-Epidermal Growth Factor Receptor-Induced Acne-Like Rash: A Randomized Left-Right Comparative Evaluation (APPEARANCE).

LESSONS LEARNED: The results of the APPEARANCE trial indicate that adapalene does not prevent acne-like rash over placebo when added to topical moisturizer and oral minocycline but instead may have a detrimental effect. Therefore, adapalene is not recommended as prophylaxis against acne-like rash induced by anti-epidermal growth factor receptor therapies.Given that acne-like rash was completely controlled with placebo in approximately half of patients, predictive measures to identify patients needing intensive prophylaxis are required.
BACKGROUND: Anti-epidermal growth factor receptor (EGFR) therapies are frequently associated with acne-like rash. To evaluate the prophylactic efficacy of adapalene, a topical retinoid used as first-line therapy for acne vulgaris, we conducted a randomized, placebo-controlled, evaluator-blinded, left-right comparative trial.
METHODS: Patients with non-small cell lung, colorectal, or head and neck cancer scheduled to receive anti-EGFR therapies were randomly assigned to once-daily adapalene application on one side of the face, with placebo on the other side. All patients had topical moisturizer coapplied to both sides of the face, and received oral minocycline. The primary endpoint was the difference in total facial lesion count of acne-like rash at 4 weeks. Secondary endpoints included complete control rate (CCR) of acne-like rash (≤5 facial lesions) and global skin assessment (Investigator's Global Assessment [IGA] scale, grade 0-4) at 4 weeks. Two blinded dermatologists independently evaluated the endpoints from photographs.
RESULTS: A total of 36 patients were enrolled, of whom 26 were evaluable. Adapalene treatment was associated with a greater lesion count than placebo at 4 weeks, although the difference was not statistically significant (mean, 12.6 vs. 9.8, p = .12). All four patients with a difference >10 in lesion count between face sides had a greater count on the adapalene-treated side. No significant differences were observed in CCR of acne-like rash (54% vs. 50%) or IGA scale (mean grade, 1.9 vs. 1.7) between the adapalene and placebo sides.
CONCLUSION: Adapalene is not recommended as prophylaxis against acne-like rash induced by anti-EGFR therapies. © AlphaMed Press; the data published online to support this summary are the property of the authors.

RCT Entities:   Population Interventions Outcomes

Discussion

Acne‐like rash is the most problematic skin toxicity induced by anti‐EGFR therapies. Although the Multinational Association for Supportive Care in Cancer (MASCC) guideline gives a grade A recommendation only for oral minocycline or doxycycline as prophylaxis for acne‐like rash induced by anti‐EGFR therapies, the development of more effective prophylactic measures is required. Because previous reports have suggested that adapalene is effective for the treatment of acne‐like rash induced by anti‐EGFR therapies, we conducted a placebo‐controlled, evaluator‐blinded, left‐right comparative trial to clarify the prophylactic effect of adapalene against the particular type of acne‐like rash.

We enrolled patients with advanced cancers, who were ≥20 years of age, with an Eastern Cooperative Oncology Group (ECOG) performance status of 0–2, and adequate organ function, and who scheduled to receive treatment with an anti‐EGFR drug (cetuximab, panitumumab, gefitinib, erlotinib, or afatinib) (Table 1).

Table 1.

Patient demographic and baseline disease characteristics

Abbreviations: ECOG, Eastern Cooperative Oncology Group; EGFR, epidermal growth factor receptor.

Although there were no statistically significant differences in any of the efficacy endpoints between adapalene‐treated and placebo‐treated sides, there was a tendency for adapalene‐treated sides to have worse outcome than placebo‐treated sides (Figs. 1, 2, 3, 4, Table 1). On the IGA scale, 15 of 26 patients scored equally between the placebo and adapalene sides, and 8 of the remaining 11 patients had a higher score on the adapalene side compared with the placebo side (Tables 3 and 4). Similarly, on the MASSC scale, whereas 16 of 26 patients had the same score for both sides, 8 of the remaining 10 patients had a greater score on the adapalene‐treated side compared with the placebo‐treated side (Tables 5 and 6).

Figure 1.

Mean facial lesion count of acne‐like rash at 0, 2, and 4 weeks of therapy.

Figure 2.

Scatter plot of differences in facial lesion count; each plot represents the difference in facial lesion count (placebo minus adapalene) in each case at 0, 2, and 4 weeks of therapy.

Figure 3.

Consolidated Standards of Reporting Trials diagram.

Figure 4.

Interval until the occurrence of acne‐like rash.

Table 3.

Dermatologists’ global assessment using the IGA scale

Based on a Wilcoxon signed‐rank test.

Abbreviation: IGA, Investigator's Global Assessment.

Table 4.

Investigator's Global Assessment Scale for acne vulgaris

Table 5.

Incidence of grade 2 or higher acne‐like rash based on the Multinational Association for Supportive Care in Cancer scale

Based on a McNemar's test.

Table 6.

Multinational Association for Supportive Care in Cancer scale for papulopustular eruption by epidermal growth factor receptor inhibitors

The most commonly observed skin adverse events other than acne‐like rash were dry skin, pruritus, pain, and erythema, and the overall incidence of each adverse event was similar between adapalene‐ and placebo‐treated sides.

To the best of our knowledge, this is the first prospective and randomized study to evaluate the prophylactic effect of adapalene against acne‐like rash induced by anti‐EGFR therapies. In contrast to our hypothesis, our findings indicate that adapalene should not be recommended for the prevention of acne‐like rash induced by anti‐EGFR therapies, although its use for the treatment of the particular type of rash may still be considered.

Trial Information

Head and neck cancers, non‐small cell lung cancer, and colorectal cancer

Metastatic / Advanced

No designated number of regimens

Phase II

Randomized

Left‐right difference (the placebo side minus the adapalene side) in total rash count after 4 weeks of therapy

IGA scale after 4 weeks

Incidence of grade ≥2 acne‐like rash based on the MASCC scale after 4 weeks

Interval to the occurrence of acne‐like rash based on patient diaries

Complete control rate of acne‐like rash defined as number of facial lesions ≤5

Incidence and severity of adverse events according to Common Terminology Criteria for Adverse Events version 4.0

Adherence based on patient diaries

Inactive because results did not meet primary endpoint

Drug Information

Adapalene gel 0.1%

Differin Gel 0.1%

Galderma

Topical retinoid

Topical application

Patient Characteristics

21

15

Median (range): 65 (47–82)

0 — 12

1 — 21

2 — 3

3 — 0

Unknown — 0

Anti‐EGFR drug: cetuximab, 12; panitumumab, 7; afatinib, 11; erlotinib, 4; gefitinib, 2. Concurrent therapy: cytotoxic agent, 18; bevacizumab, 2; monotherapy, 16

Non‐small cell lung cancer, 17; colorectal cancer, 14; head and neck cancer, 5

Primary Assessment Method

Primary analysis

36

36

35

26

Left‐right difference (the placebo side minus the adapalene side) in total rash count after 4 weeks of therapy

Mean lesion count, adapalene‐treated versus placebo‐treated sides, 12.6 versus 9.8, p = .12

Adverse Events: Adapalene Side

Adverse Events: Placebo Side

Assessment, Analysis, and Discussion

Study completed

Inactive because results did not meet primary endpoint

Anti‐epidermal growth factor receptor (EGFR) therapies, either anti‐EGFR monoclonal antibodies (MABs) or EGFR tyrosine kinase inhibitors (TKIs), are commonly used to treat patients with colorectal, non‐small cell lung, pancreatic, and head and neck cancers. The acne‐like rash that develops mainly on the face and trunk is a particularly problematic toxicity of anti‐EGFR therapies because it occasionally leads to diminished quality of life in patients and treatment interruption [1], [2]. Additionally, the severity of the acne‐like rash has been reported to correlate with the therapeutic effects of anti‐EGFR drugs in some types of cancer [3], [4]. It is therefore critical to optimize the prophylactic management of the acne‐like rash induced by these treatments.

Several randomized trials have shown that tetracyclines such as doxycycline and minocycline are useful as prophylaxis against skin toxicity caused by anti‐EGFR therapies [5], [6]. For example, prophylaxis with a topical steroid and oral doxycycline was shown to reduce the incidence of grade ≥2 skin toxicities induced by panitumumab, compared with the same treatment given in a reactive manner in the Skin Toxicity Evaluation Protocol with Panitumumab (STEPP) trial [6]. Based on these findings, the Multinational Association for Supportive Care in Cancer (MASCC) guideline gives a grade A recommendation for the use of oral minocycline 100 mg daily or doxycycline 100 mg twice daily as prophylaxis for acne‐like rash induced by anti‐EGFR therapies [7]. However, the recommendation for prophylaxis with topical hydrocortisone 1% cream remains at grade C [7]. Because regular use of topical corticosteroids can cause various forms of skin toxicity such as skin atrophy and telangiectasia, development of other prophylactic therapies is required.

Adapalene, a naphthoic acid derivative that is used to treat acne vulgaris, has high affinity toward retinoic acid receptors β and γ and may normalize keratinocyte proliferation and differentiation and reduce inflammation [8]. Some case reports and case series have shown that adapalene is effective for the treatment of acne‐like rash induced by anti‐EGFR therapies [9], [10], [11]. In a Japanese phase II trial, the incidence of grade ≥2 skin toxicities during 6 weeks of prophylactic therapy with topical adapalene and oral minocycline in patients receiving panitumumab was 29.2%, and it was similar to that in the STEPP trial [12]. To date, however, the prophylactic effect of adapalene has not been adequately evaluated, and we therefore conducted the present study. Adapalene unexpectedly did not demonstrate a prophylactic effect on acne‐like rash induced by anti‐EGFR therapies when coadministered with topical moisturizer and oral minocycline, but instead appeared to have a detrimental effect compared with placebo.

The study design comparing the sides of a patient's face can eliminate background differences and enable the sample size to be minimized. We used the base of the 0.1% adapalene gel (Differin Gel, Galderma, La Defense, France) as the placebo. Because tiny particles of adapalene can be visualized in the gel, this study was not strictly double‐blinded but instead was evaluator‐blinded. The dermatologists evaluated the skin condition based on photographic images without seeing the patients and thus minimized the risk of bias.

A somewhat detrimental effect of topical retinoic acid receptor‐specific retinoid as prophylaxis for acne‐like rash was not entirely unexpected. In a previous study, tazarotene 0.05% cream, another retinoid, was applied to one half of the face only, starting from initiation of cetuximab treatment [5]. Although there were fewer skin eruptions, on average, in the tazarotene group, global assessment by a dermatologist at week 4 was equivalent for both sides in 87% of patients but worse for tazarotene‐treated sides in 10% of patients. However, in 14 out of 43 patients (32.6%), tazarotene application was interrupted because of local irritation. We therefore suggest that the unsuccessful outcome of tazarotene prophylaxis might have been attributable to skin‐irritating toxicity. We used adapalene in the present study because it is less irritating than tazarotene [13], and evidence of its effect on EGFR inhibitor‐induced acne‐like rash is accumulating [10], [11], [12]. Based on our results, however, adapalene might still have had an irritating effect and render the skin more susceptible to acne‐like rash compared with placebo. Our findings, however, do not negate the effect of adapalene for the treatment of acne‐like rash induced by anti‐EGFR therapies. When used for the treatment of acne‐like rash, adapalene is applied as a dot onto each lesion rather than in a planar fashion, as used for prophylactic purposes, and therefore might not irritate normal skin around the lesion.

We estimated that there would be 30 facial lesions on the placebo side based on a study with mainly white subjects, but there were fewer lesions in our study, with a mean of 9.8. Additionally, the complete control rate on the placebo side was 50%, and 42% and 46% of patients had grade 0 or 1 IGA scale and grade 1A or 1B MASCC scale on the placebo side, respectively. This may indicate that East Asians are less susceptible to anti‐EGFR therapies, and that a topical moisturizer and oral minocycline may be sufficient treatment for approximately half of the patients. However, the remaining patients may still require prophylactic measures to prevent the development of an acne‐like rash.

Our study had several limitations. First, although we evaluated patients who received different EGFR‐TKIs and EGFR‐MABs together, pathology and the response to adapalene may differ between acne‐like rashes depending on the causative agent. In our study, three of four patients with a facial lesion count of >10 on the adapalene‐treated side compared with the placebo‐treated side received an EGFR‐TKI (afatinib for one patient and erlotinib for two patients). Second, because there is no standardized method for lesion counting, the generalizability of our results is limited. However, there was a high consistency in the lesion count by the two evaluators in the present study (Cronbach's coefficient alpha >0.9).

In conclusion, our findings indicate that adapalene should not be recommended for the prevention of acne‐like rash induced by anti‐EGFR therapies. Predictive measures to identify patients needing intensive prophylaxis over topical moisturizer and oral minocycline are required. There is also a requirement for more effective and less toxic prophylactic agents than topical corticosteroids.

Although the overall incidence of each adverse event was similar between adapalene‐ and placebo‐treated sides, some grade 2 events were observed only on adapalene‐treated sides.

Abbreviation: NC/NA, no change from baseline/no adverse event.

Abbreviation: NC/NA, no change from baseline/no adverse event.

Table 2.

Rates of complete control of acne‐like rasha

Determined as (the number of faces with an acne‐like rash count of 5 or less) / (total number of faces in the efficacy analysis population).

Based on a McNemar's test.