Pharmacotherapeutic group: Other dermatological preparations, antihidrotics, ATC code: D11AA01
Mechanism of action
Glycopyrronium is a competitive antagonist of the muscarinic acetylcholine receptors.
Pharmacodynamic effects
Glycopyrronium inhibits acetylcholine-driven effects on smooth muscle and heart muscle cells and on various glands, including the sweat glands. In the sweat glands, this results in a reduction in perspiration.
Clinical efficacy and safety
The safety and efficacy of Axhidrox in patients with primary axillary hyperhidrosis was evaluated in a Phase 3 Study, consisting of a 4-week double-blind and placebo-controlled treatment period (Phase 3a Part), followed by an open-label extension of treatment up to 72 weeks (Phase 3b Part).
In total, 171 patients (18-65 years) were included in the 4-week, multicentre, randomized, double-blind, placebo-controlled Phase 3a Part of the pivotal study. Across the treatment groups, the mean age was 36 years, 51% were men. Almost all were of white ethnic origin. The disease severity was severe primary axillary hyperhidrosis (HDSS score of 3 or 4) with at least 50 mg of sweat production in each axilla measured gravimetrically at room temperature and at a humidity consistent with the normal climate in that area over a period of 5 minutes.
The primary endpoint was defined as the absolute change in sweat production with the GPB 1% cream vs. placebo from baseline to Day 29, as assessed by gravimetry. Key secondary endpoints were the comparison between GPB 1% cream and placebo regarding absolute change in Hyperhidrosis Quality of Life Index (HidroQoL) score from baseline to Day 29 and the percentage of responders based on HDSS score at Day 29 (improvement of ≥ 2 points).
After 4 weeks of treatment in the placebo-controlled Phase 3a Part, the group treated with Axhidrox showed a larger, approximately 2-fold, sweat reduction from baseline than the placebo group. The absolute reduction in sweat production from baseline to Day 29 was statistically significantly higher in the Axhidrox group compared with the placebo group (Table 2).
The analysis assessing the key secondary endpoints showed an improvement of 2 or more points in the HDSS score to treatment with Axhidrox than to treatment with placebo (p = 0.0542). In the analysis assessing absolute changes in the HidroQoL score, the median improvement was significantly larger in the group treated with Axhidrox than with placebo group (p < 0.0001).
Table 2. Data from the Phase 3a Part
| | Placebo (n = 84) | GPB 1% (n = 87) | GPB 1% vs. placebo p-values |
| Primary endpoint |
| Absolute change in sweat production from Baseline to Day 29 |
| Baseline [mg] (mean ± SD) | 284.64 (212.47) | 306.97 (249.33) | – |
| Change to Day 29 [mg] (mean ± SD) | –83.49 (168.21)a | –197.08 (252.41)b | 0.0038 |
| Relative change to Day 29 [%] Median (95% CI) | -34.32 (-49.71; -2.67)a | -64.63 (-73.13; -51.75)b | < 0.0001 |
| Sweat reduction of ≥ 50%, vs baseline (number of patients, (%)) | 29 (34.5) | 50 (57.5) | 0.0114 |
| Key secondary endpoints |
| HDSS responders (≥2-point improvement from Baseline to Day 29) |
| Responder rate, N (%) | 10 (11.9) | 20 (23.0) | 0.0542 |
| Change in the HidroQoL from Baseline to Day 29 |
| Total score, median (range) Change to Day 29 | -1.0 (-35 - 4)c | -6.0 (-36 - 6)d | < 0.0001 |
HDSS = Hyperhidrosis Disease Severity Scale, HidroQoL = Hyperhidrosis Quality of Life Index, CI = confidence interval, N = number of patients, aN=78, bN=77, cN=79, dN=84.
In the open-label long-term Phase 3b Part, sweat production was significantly reduced compared to baseline 4 and 12 weeks after treatment with Axhidrox (N = 357 newly recruited patients; p < 0.0001 for both week 4 and 12) (Table 3).
Table 3. Data from the Phase 3b Part
| Primary endpoint (only newly recruited patients) | | vs. baseline |
| Absolute change in total sweat production assessed by GM from Baseline (Day 1b) to Week 12. |
| Baseline [mg] (mean ± SD) (n = 357) | 280.31 (238.24) | |
| Week 12 [mg] (mean ± SD) (n = 316) | 123.64 (149.06) | < 0.0001 |
| Secondary efficacy endpoints (sweat reduction): | | |
| Sweat reduction of ≥ 50%, vs baseline (number of patients, (%)) Week 4 | 198 (55.5) | |
| Sweat reduction of ≥ 50%, vs baseline (number of patients, (%)) Week 12 | 193 (54.1) | |
| Key secondary endpoints (N=518) | | |
| HDSS responders (≥ 2-point improvement from Baseline to Week 12) - > 25% responders |
| Responders, N (%) | 145 (30.8) | 0.0019 |
| HDSS responders (≥ 2-point improvement from Baseline to Week 28) - > 25% responders |
| Responders, N (%) | 152 (29.3) | 0.0112 |
| Absolute change in the hyperhidrosis quality of life index HidroQoL from Baseline to Week 12 |
| Total score Median change to Week 12 (CI) | -11.0 (-13.0; -10.0)a | < 0.0001 |
HDSS = Hyperhidrosis Disease Severity Scale, HidroQoL = Hyperhidrosis Quality of Life Index, CI = confidence interval, N = number of patients, aN=468
Percentage of responders (≥ 2 points improvement in HDSS) did not reach statistical significance (p = 0.0623) after 4 weeks of treatment with Axhidrox in the open-label, long-term Part of the Phase 3 Study (N = 357 patients) with Axhidrox. However, statistical significance was reached after 52 (p = 0.0072) and 72 (p < 0.0002) weeks of treatment with Axhidrox. Absolute changes in the total HidroQoL score from baseline were statistically significant on week 4, 8, 28, 52 and 72 (p < 0.0001 for all) after treatment with Axhidrox.
Patient reported outcomes, such as HDSS and HidroQoL, showed a further improvement over time despite reduction of application frequency after week 4. The hyperhidrosis symptoms ameliorated further with long-term use for up to 72 weeks of treatment.
The European Medicines Agency has deferred the obligation to submit the results of studies with Axhidrox in one or more subsets of the paediatric population in condition, as per paediatric investigation plan (PIP) decision, for the granted indication (see section 4.2 for information on paediatric use).