Effectiveness of the capsaicin 8% patch in the management of peripheral neuropathic pain in European clinical practice: the ASCEND study

The ASCEND study (NCT01737294) was a Phase 4, multi-centre, open-label, non-interventional study (NIS) conducted between February 2012 and August 2014 in accordance with the principles of the Declaration of Helsinki, International Conference on Harmonisation Guidelines, and local ethical and legal requirements.

Patients were eligible for inclusion if they were at least 18 years old, recommended capsaicin 8% patch treatment by their treating physician, diagnosed with non-diabetic PNP and had provided written informed consent for participation in the study. Patients were excluded for the following reasons: neuropathic painful areas located only on the face, above the hairline of the scalp and/or in proximity to mucous membranes; history of diabetes mellitus; diagnosis of any major psychiatric disorder, or evidence of cognitive impairment; prior treatment with capsaicin 8% patch; hypersensitivity to capsaicin, capsaicin 8% patch excipients/adhesives, and/or local anaesthetics; participation in any other clinical study and/or receipt of an investigational drug within 30 days prior to screening visit; history of substance abuse (including alcoholism).

A detailed medical history was taken with particular emphasis on the primary PNP diagnosis. Patients were classified into one of six aetiology groups: PHN; HIV-AN; neuropathic back pain (NBP), including cases secondary to radiculopathy, polyneuropathy, plexopathy and ankylosing spondylitis; cancer-related neuropathic pain (CRNP); post-operative and post-traumatic neuropathic pain (PONP); ‘other’ neuropathies. Prior and concomitant medications were recorded at baseline and patients were categorised by the treating physician as being in the primary (first treatment received for NP), secondary (second treatment received for NP) or tertiary (at least third treatment received for NP) stage of the treatment pathway. The duration of pre-existing PNP was recorded.

Study medication was prescribed in routine clinical practice. At each treatment visit, the size and location of the patient’s painful area was assessed to determine the required area of treatment. Each capsaicin 8% patch contained 179 mg of capsaicin (640 μg per 1 cm²) and up to four patches were allowed per treatment. Multiple treatment areas were possible; the recommended treatment time was 30 min for the foot and 60 min for other anatomical sites. Patients were followed up by phone or during clinic visits (Fig. 1). Scheduled follow-up contact at Week 2 and Week 8 was made after first treatment only. Subsequent follow-up contact was made at Week 12, Week 26, Week 39 and Week 52. Multiple treatments with the capsaicin 8% patch were allowed, although intervals of at least 90 days between each application were recommended, consistent with the summary of product characteristics [20].

Patients assessed the intensity of their pain using an 11-point numeric pain rating scale (NPRS) ranging from 0 (no pain) to 10 (worst imaginable pain) [21]. NPRS ‘average pain during the last seven days’ score was recorded at the screening visit and used as baseline pain in all related analyses. NPRS ‘average pain during the last 24 h’ score was recorded at each treatment visit/assessment (prior to patch application). Sensitivity analysis was performed to exclude the effect of treatment outside of the recommended application time (<90% and ≥110%) on the pain response. HRQoL was assessed using the EuroQol 5 Dimension 3-level (EQ-5D) questionnaire [22]. The default York MVH A1 value set [23] was used to derive the EQ-5D index for all observations in this study. The change in patients’ general state of health was assessed by the patient global impression of change (PGIC) instrument [24] using a 7-point Likert scale, ranging from 1 (very much improved) to 7 (very much worse). Patients were asked to indicate how they felt ‘now’, compared with how they felt before receiving their most recent capsaicin 8% patch treatment.

The primary endpoints were: (i) the percentage change in mean NPRS ‘average pain’ score from baseline to the average of Weeks 2 and 8 following first capsaicin 8% patch treatment; and (ii) the median time between the first and second capsaicin 8% patch treatments. Secondary endpoints were: the percentage change in mean NPRS score from baseline to the average of Weeks 2 and 12 following re-treatment(s); the proportion of patients with a ≥30% or ≥50% reduction in mean NPRS score from baseline to the average of Weeks 2 and 8 for first treatment or the average of Weeks 2 and 12 for re-treatment (defined as ≥30% responders and ≥50% responders, respectively); the percentage change in mean NPRS scores from baseline to each assessment; median time between second and third treatment; number of capsaicin 8% patches used at each treatment; treatment area size at each treatment; the proportion of patients completing ≥90% of the recommended treatment duration at each application (≥27 min for the feet or ≥54 min for all other anatomical sites); change in EQ-5D index from baseline to each assessment; proportion of patients with improved overall health status versus baseline according to the PGIC (i.e. very much improved, much improved or slightly improved) at assessments; proportion of patients reporting adverse events (AEs) and serious AEs (SAEs). All study assessments were performed at scheduled follow-up visits and, with the exception of EQ-5D, at additional, unscheduled visits.

All analyses were performed using the full analysis set (FAS), consisting of all patients who received treatment with the capsaicin 8% patch. The planned primary analysis was to test equivalence between the PHN group and each of the other PNP aetiology groups for each co-primary endpoint. The margin of equivalence for percentage change in mean NPRS score was set at ±16% (comparable to a one-point change on the NPRS scale [25]) while for time to re-treatment, it was set at ±1 month according to clinical judgement. The decision to perform inferential equivalence testing between the patients in the PHN aetiology group and those in any of the other PNP aetiology groups for the analysis of the co-primary endpoints was based on the number of PHN patients recruited and the minimum number of patients in any one of the other aetiologies required to achieve 80% power.

A total of 429 patents were enrolled in the study and 420 patients received at least one treatment with the capsaicin 8% patch (FAS). Patients were from seven European countries: Austria (7 sites, n = 65), Greece (11 sites, n = 88), Italy (8 sites, n = 30), Portugal (11 sites, n = 98), Spain (7 sites, n = 68), Switzerland (2 sites, n = 22) and United Kingdom (5 sites, n = 49). The median age of the study population was 61 (range 21–98) years; 39.8% of patients were male; and the most common diagnoses were PONP (47.1%, n = 198) and PHN (21.1%, n = 89) (Table 1). The proportion of patients in the primary, secondary or tertiary stage of the treatment pathway was 19.3%, 42.9% and 37.9%, respectively. Overall, patients had a median follow-up time of 370 days (interquartile range: 360–434).

At first treatment, the mean number of patches used was 1.5 (standard deviation [SD] ±0.7) and the mean treatment area was 306.4 (SD ±228.2) cm²; both values remained consistent through successive applications (Table 2). A total of 239 (56.9%) patients received only one treatment with the capsaicin 8% patch, 181 (43.1%) patients received at least two treatments and 70 (16.7%) patients received at least three treatments. At first treatment, patches were applied to the following body areas: legs (36.2%, n = 152); torso (35.0%, n = 147); feet (16.2%, n = 68); hands (8.6%, n = 36); arms (8.3%, n = 35); and the head and neck (5.5%, n = 23), excluding areas above the hairline of the scalp and/or in proximity to mucous membranes. During first treatment, 388 patients (92.4%) completed ≥90% of the recommended duration of patch application. Similarly, 157 (94.0%) and 63 (98.4%) patients completed ≥90% of the recommended duration of patch application at second and third treatment, respectively.

Following first treatment with the capsaicin 8% patch, there was an overall 26.6% (95% CI: 23.6, 29.6; n = 412) reduction in mean NPRS ‘average pain’ score from baseline to Weeks 2 and 8 (co-primary endpoint) (Table 3; Fig. 2a). The findings of the sensitivity analysis were consistent with this result (–27.7%; n = 254). The primary analysis demonstrated equivalence between the PHN group and each of NBP, PONP and ‘other’ groups as the difference did not exceed the pre-defined margin of equivalence (Fig. 2a). Patients who received second and third treatments had similar reductions in their mean NPRS scores of 28.7% (95% CI: 22.9, 34.5; n = 161) and 27.3% (95% CI: 18.1, 36.5; n = 59), respectively from baseline to Weeks 2 and 12. Overall, patients had a 24.5% (95% CI: 21.1, 27.9; n = 401) reduction in their mean NPRS score from baseline to Week 2 and a 37.0% (95% CI: 31.3, 42.7; n = 176) reduction to Week 52 (Fig. 2b).

A total of 44.4% (n = 183) and 26.2% (n = 108) of patients were classified as ≥30% and ≥50% responders, respectively, after first treatment (Table 4). Of responders at Week 8, 86.9% (n = 159/183) retained responder status at Week 12 after first treatment. There was a small increase in the percentage of responders following re-treatment. The percentage of ≥30% responders after second and third treatment was 49.1% (n = 79) and 49.2% (n = 29), respectively (Table 4). The percentage of ≥50% responders at second and third treatment was 30.4% (n = 49) and 30.5% (n = 18), respectively. These findings suggest that the proportion of responders was maintained with each subsequent capsaicin 8% patch treatment.

In a subgroup analysis, patients in the shortest PNP duration quartile of 0–0.72 years had a 36.3% (95% CI: 30.0, 42.6; n = 101) reduction in their mean NPRS score from baseline to Weeks 2 and 8 compared with reductions of 23.6% (95% CI: 17.1, 30.1; n = 104), 25.0% (95% CI: 19.4, 30.6; n = 104), and 21.8% (95% CI: 16.4, 27.2; n = 103), in the 0.72–2.1 years, >2.1–5.4 years and >5.4 years quartiles, respectively. Similarly, 62.4% of patients in the shortest PNP duration quartile (0–0.72 years) were ≥30% responders after first treatment, followed by 39.4% of patients in 0.72–2.1 years, 40.4% in >2.1–5.4 years, and 35.9% in >5.4 years PNP duration quartiles, respectively. In patients classified as being in the primary, secondary and tertiary stages of the treatment pathway, the change in mean NPRS scores from baseline to Weeks 2 and 8 was –30.5% (n = 80), –28.1% (n = 177), and –22.8% (n = 155), respectively.

Patients had a median time from first to second treatment of 191 days (95% CI: 147, 235; n = 181) (co-primary endpoint) and a median time from second to third treatment of 301 days (95% CI: 245, 357; n = 70) (Fig. 3a). The median time to second treatment for the PHN and PONP groups was 180 days (95% CI: 116, 244; n = 40) and 161 days (95% CI: 120, 202; n = 97), respectively (Fig. 3b). Median time to second treatment could not be calculated for NBP and the ‘other’ aetiology groups within the period of the study and the HIV-AN and CRNP aetiology groups were excluded due to low recruitment.

The mean EQ-5D health state utility score increased by 0.199 utils at Week 2 (from a baseline score of 0.345 utils), at least two-times greater than the minimally important difference of 0.074 utils [26]. This improvement was maintained to Week 52 following first treatment (Table 5). Responders to capsaicin 8% patch treatment reported the most substantial improvements in HRQoL. At Week 2 after first treatment, ≥30% and ≥50% responders had increases of 0.292 utils and 0.327 utils, respectively in their EQ-5D scores from baseline.

Analysis of PGIC demonstrated that the majority of patients experienced an improvement (very much, much or slightly) in health status during the study (Table 6). Following first, second and third treatment applications, 61.0% (n = 224/367), 74.6% (n = 112/150) and 78.7% (n = 37/47) of patients, respectively reported improved status at Week 12, while 7.4% (n = 27/367), 5.3% (n = 8/150) and 4.3% (n = 2/47) of patients reported some deterioration. At Week 52, following first, second or third treatment, more than half of all patients had an improvement in PGIC and less than 8% had worsened.

Capsaicin 8% patch treatment was generally well tolerated. Over the course of the study, 47 (11.2%) patients reported a total of 91 AEs. The number of patients reporting at least one AE following first, second, third and fourth treatment was 26 (6.2%), 15 (3.6%), 5 (1.2%) and 1 (0.2%), respectively. The most frequently reported AEs were anticipated capsaicin-related application site reactions (8.3%; n = 35) including erythema (8.1%; n = 34), pain (5.0%; n = 21) and pruritus (1.0%; n = 4). Twenty-one SAEs were reported in 9 (2.1%) patients; five of these reported for one patient were probably treatment-related (two application site erythema, two application site pruritus and one headache). Four patients died during the study; causes of death were assessed by the treating physicians and were not considered to be treatment-related.