Pharmacotherapeutic group: Antihemorrhagics, other systemic haemostatics. ATC code: B02BX09
Mechanism of action
Fostamatinib mediates its activity effectively through its major metabolite, R406, which is a tyrosine kinase inhibitor with demonstrated activity against spleen tyrosine kinase (SYK). R406 inhibits signal transduction of B-cell receptors and Fc-activating receptors, which play a key role in antibody-mediated cellular responses. The fostamatinib metabolite R406 reduces antibody-mediated destruction of platelets.
Clinical efficacy and safety
The efficacy and safety of fostamatinib has been demonstrated in two Phase III, randomised, double-blind, placebo-controlled studies (C788-047 and C788-048) in adult patients with previously treated persistent (3-12 months since diagnosis) or chronic (greater than 12 months since diagnosis) ITP.
Randomised, placebo-controlled studies
A total of 150 patients with persistent or chronic ITP, who had an insufficient response to previous treatment (which included corticosteroids, immunoglobulins, splenectomy, and/or a thrombopoietin receptor agonists) were enrolled in two identical, double-blind, placebo-controlled studies that were conducted in different countries.
For each study, patients were randomised 2:1 to fostamatinib or placebo for 24 weeks; randomisation was stratified with respect to prior splenectomy and severity of thrombocytopenia. Stable concurrent ITP therapy (glucocorticoids [less than 20 mg prednisone equivalent per day], azathioprine, or danazol) was allowed, and rescue therapy was permitted, if needed. All patients initially received study medicinal product at 100 mg twice daily (or matching placebo). Based on platelet count and tolerability, dose escalation to 150 mg twice daily (or matching placebo) was undertaken in 86% of patients at Week 4 or later.
Patients enrolled in the placebo-controlled studies had a median age of 54 years old (range: 20 to 88 years; median age in C788-047 was 57.0 and in C788-048 was 49.5 years), and the majority were female (61%) and were white (93%). Prior ITP treatments were varied (median of 3, range of 1-14), with the most common including corticosteroids (94%), immunoglobulins (53%), and thrombopoietin receptor agonists (TPO-RA) (48%). Most patients had chronic ITP (93%), with a median time since ITP diagnosis of 8.5 years, and 35% had undergone splenectomy. At baseline, the median platelet count was 16 000/µL (with almost half [45%] less than 15 000/µL) and 47% were on stable ITP therapy. Of the 102 patients with ITP who received fostamatinib, 28 (27%) were 65 years of age and older while 11 (11%) were 75 years of age and older.
In Study C788-047, 76 patients were randomised; 51 to the fostamatinib group and 25 to the placebo group. In Study C788-048, 74 patients were randomised; 50 to the fostamatinib group and 24 to the placebo group. The efficacy of fostamatinib was based on the primary endpoint of stable platelet response (at least 50 000/µL on at least 4 of the 6 visits between Weeks 14 to 24). Study outcomes for C788-047 and C788-048 are shown in table 4.
Table 4: Study outcomes from placebo-controlled clinical studies
| Study Outcomes | Statistical Parameters | Study C788-047 | Study C788-048 | Pooled studies | Refractory population6 |
| Fosta (N=51) | PBO (N=25) | Fosta (N=50) | PBO (N=24) | Fosta (N=101) | PBO (N=49) | Fosta (N= 72) | PBO (N=33) |
| Stable platelet response1,2 | n (%) | 8 (16) | 0 (0) | 9 (18) | 1 (4) | 17 (17) | 1 (2) | 10 (14) | 0 (0) |
| CI 95% | (5.7, 25.7) | (0, 0) | (7.4, 28.7) | (0, 12.2) | (9.5, 24.1) | (0, 6.0) | (5.9, 21.9) | (0.0, 0.0) |
| p-value | p3 = 0.0471 | NS | p3=0.0071 | P3=0.0287 |
| Eligible for C788-0494 at Week 125 | n (%) | 28 (55) | 22 (88) | 33 (66) | 19 (79) | 61 (60) | 41 (84) | 43 (60) | 29 (88) |
| Completed study (Week 24) | n (%) | 12 (24) | 1 (4) | 13 (26) | 2 (8) | 25 (25) | 3 (6) | 16 (22) | 1 (3) |
1 Includes all patients with platelet counts and excludes patients whose platelet counts were measured following rescue therapy after Week 10.
2 Stable platelet response was prospectively defined as a platelet count of at least 50 000/µL on at least 4 of the 6 visits between Weeks 14 and 24.
3 p-value from Fisher Exact test
4 C788-049: open label extension study
5 Patients who did not respond to treatment after 12 weeks were eligible to enrol in open-label extension study.
6 Refractory patient population defined as the subgroup of patients who had received three or more prior other ITP therapies
Fosta = fostamatinib; PBO = placebo; NS = Did not demonstrate a statistically significant difference between treatment arms
An initial therapeutic response (platelet count ≥ 50 000/μL) was observed within 6 weeks for most responders (11 of 17 responders) and within 12 weeks for all stable responders.
Among patients who were stable responders, the median platelet count increased to 95 000/µL across post-baseline visits with a maximum of 150 000/µL. Rescue medicinal product was required by 30% and 45% of patients receiving fostamatinib or placebo, respectively.
During the placebo-controlled studies, the incidence of bleeding occurred in 29% and 37% of patients in the fostamatinib and placebo arms, respectively. The incidence of moderate or severe bleeding‑related adverse events (AEs) (16.3% vs. 9.9%) and serious adverse events (SAEs) (10.2% vs 5.0%) was about twice as high in the placebo group compared with the fostamatinib group. Only one subject treated with fostamatinib experienced a severe bleeding-related event (contusion), while three subjects treated with placebo experienced severe events (gastrointestinal haemorrhage, menorrhagia and petechiae). In sum, there were trends for reduced bleeding-related AEs with fostamatinib compared to placebo; differences between the groups were not statistically significant.
Subset analyses
Platelet count responses for patients treated with TAVLESSE were further analysed as shown in table 5. Results are shown for both the pooled population (from Studies C788-047 and C788-048) and a refractory patient population defined as the subgroup of patients who had received three or more prior other ITP therapies. For all platelet count parameters, the results for the pooled population are comparable to the refractory patient population.
Table 5: Summary of platelet count parameters by subgroup – pooled patient population (C788-047 and C788‑048) and refractory patient population
| Parameters | Pooled population Fostamatinib N=101 | Refractory patient population Fostamatinib N=72 |
| Subject with platelet response (≥50000/µL) at Week 12, n (%) |
| Yes | 23 (22.8%) | 14 (19.4%) |
| No | 78 (77.2%) | 58 (80.6%) |
| Change from baseline in platelet count (/µL) at Week 12 |
| Median | 4 000 | 3 000 |
| Range | (-15 000, 220 000) | (-5000, 159000) |
| Median platelet count (/µL) Over Time |
| Median | 22 000 | 16 750 |
| Range | (1 000, 254 500) | (1 000, 105 500) |
Extension Study
The C788-049 trial is an open label extension study. Patients from C788-047 and C788-048 who completed 24 weeks of treatment, or who did not respond to treatment after 12 weeks, were eligible to enrol in this study. Patients remained blinded to their treatment assignment from the previous study (fostamatinib or placebo), so their starting dose in this study was based on their final platelet count.
For the C788-049 trial, 123 patients were enrolled, 44 patients previously randomised to placebo and 79 patients previously randomised to fostamatinib.
Placebo Crossover: In a prospectively defined analysis, the 44 subjects treated with placebo in the prior study were evaluated for stable response for fostamatinib (from the first 24 weeks of the study) with their placebo data as the comparator for this objective measure. Ten of these subjects (22.7%) (including a single subject who was classified as a placebo responder in the prior study) met the criteria for stable response. Thus, the difference in response from fostamatinib compared with placebo was 20.5% (95% CI = 8.5-32.4).
Extension: Among the patients who achieved stable response in C788-047, C788-048 and C788-049 studies, 18 subjects maintained the platelet count of at least 50,000/µL for 12 months or longer.
Paediatric population
The European Medicines Agency has waived the obligation to submit the results of studies with fostamatinib in all subsets of the paediatric population for the treatment of thrombocytopenia for patients with chronic immune thrombocytopenia (ITP), who have had an insufficient response to a previous treatment (e.g., corticosteroids), (see section 4.2 for information on paediatric use).