Abstract
Abstract 2225
IB1001 is a recombinant factor IX product being investigated for the treatment and prevention of bleeding in individuals with hemophilia B. Pharmacokinetics (PK) in adults (>12 years) demonstrated that IB1001 had results similar to the currently available recombinant FIX with respect to parameters such as terminal phase half-life and incremental recovery.
We report the interim findings from a PK assessment in children <12 years, with severe hemophilia B (FIX <2%), >50 prior exposure days to FIX, and no history of or currently detectable inhibitor to FIX.
Non-randomized, open-label PK study with patients receiving 75±5 IU/kg of IB1001 following a washout period of ≥4 days from a previous FIX infusion. Factor IX levels were determined pre-infusion and at 15–30 minutes, 4–6, 24–26, and 68–72 hours post-infusion. Additional samples could be drawn at 1–3 and 10–14 hours.
Calculated PK parameters were: half-life (β-phase t1/2, determined using a robust regression approach [Lee ML et al. XVIth ISTH Congress, Florence, Italy, 1997]) but generally assuming a single compartmental model because of the small number of points, maximum plasma concentration (Cmax), in vivo recovery (IVR) and AUC(0-∞) (determined by the trapezoidal rule). In addition, the AUC(0-t) and mean residence time (MRT) were calculated.
| Subject . | t 1/2 α (hr) . | t 1/2 β (hr) . | MRT (hr) . | Cmax (IU/dl) . | In vivo Recovery (IU/dl) . | AUC0-∞ (IU/dl/hr) . | AUC0-t (IU/dl/hr) . | Age (years) . |
|---|---|---|---|---|---|---|---|---|
| Subjects 6 - 12 Years of Age . | ||||||||
| 32001 | n/a | 17.7 | 22 | 63 | 0.84 | 1461 | 1359 | 9 |
| 12001 | n/a | 17.5 | 21.2 | 57 | 0.76 | 1138 | 1062 | 7.5 |
| 32003 | 7 | 20.7 | 24 | 58 | 0.77 | 1067 | 977 | 11.1 |
| 35002 | n/a | 33.6 | 55 | 22 | 0.29 | 605 | 410 | 10 |
| mean±SD (median) | 22.4±7.6 (19.2) | 30.6±16.3 (23) | 50±19 (57.5) | 0.66±0.25 (0.765) | 1068±353 (1102.5) | 952±397 (1019.5) | 9.4±1.5 (9.5) | |
| Subjects < 6 Years of Age | ||||||||
| 4001 | n/a | 7.6 | 12.1 | 60 | 0.8 | 942 | 941 | 2 |
| 35001 | n/a | 16.3 | 19.5 | 64 | 0.85 | 1217 | 1147 | 4 |
| 32002 | n/a | 21.9 | 29.4 | 40 | 0.53 | 986 | 870 | 4.5 |
| mean±SD (median) | 15.3±7.2 (16.3) | 20.3±8.7 (19.5) | 55±13 (60) | 0.73±0.17 (0.8) | 1048±148 (986) | 986±144 (941) | 3.5±1.3 (4) | |
| Subject . | t 1/2 α (hr) . | t 1/2 β (hr) . | MRT (hr) . | Cmax (IU/dl) . | In vivo Recovery (IU/dl) . | AUC0-∞ (IU/dl/hr) . | AUC0-t (IU/dl/hr) . | Age (years) . |
|---|---|---|---|---|---|---|---|---|
| Subjects 6 - 12 Years of Age . | ||||||||
| 32001 | n/a | 17.7 | 22 | 63 | 0.84 | 1461 | 1359 | 9 |
| 12001 | n/a | 17.5 | 21.2 | 57 | 0.76 | 1138 | 1062 | 7.5 |
| 32003 | 7 | 20.7 | 24 | 58 | 0.77 | 1067 | 977 | 11.1 |
| 35002 | n/a | 33.6 | 55 | 22 | 0.29 | 605 | 410 | 10 |
| mean±SD (median) | 22.4±7.6 (19.2) | 30.6±16.3 (23) | 50±19 (57.5) | 0.66±0.25 (0.765) | 1068±353 (1102.5) | 952±397 (1019.5) | 9.4±1.5 (9.5) | |
| Subjects < 6 Years of Age | ||||||||
| 4001 | n/a | 7.6 | 12.1 | 60 | 0.8 | 942 | 941 | 2 |
| 35001 | n/a | 16.3 | 19.5 | 64 | 0.85 | 1217 | 1147 | 4 |
| 32002 | n/a | 21.9 | 29.4 | 40 | 0.53 | 986 | 870 | 4.5 |
| mean±SD (median) | 15.3±7.2 (16.3) | 20.3±8.7 (19.5) | 55±13 (60) | 0.73±0.17 (0.8) | 1048±148 (986) | 986±144 (941) | 3.5±1.3 (4) | |
When compared to the findings previously reported with IB1001 in adult (≥12 years of age) subjects (Martinowitz U et al. Haemophilia, 18, 2012), the results in pediatric patients demonstrate a more rapid metabolism of factor IX as is indicated by the shorter terminal half-life (mean±SD of 19.3±7.8 h versus 29.6±18.2 h in adults) and the smaller AUC0-∞ (mean±SD of 1059±264 versus 1668±598 in adults). In addition, the in vivo recovery was lower (mean±SD of 0.69±0.21) versus that seen in adults (mean±SD of 0.98±0.22). These results are similar to those reported by Berntorp et al (Haemophilia, 7, 2001) with nonacog alfa.
The pharmacokinetics of IB1001 has previously been shown to be non-inferior to nonacog alfa, another recombinant factor IX, in hemophilia B individuals >12 years of age. The current study is intended to provide information on children <12 and, particularly, <6 years of age. IB1001 is metabolized faster and has a lower recovery than the comparable findings in patients >12 years of age. Although the study is ongoing, these may represent important implications for the potential use of IB1001 in pediatric patients.
Gomperts:Inspiration Biopharmaceuticals Inc: Consultancy. Apte:Inspiration Biopharmacauticals Inc: Research Funding. Chaudhuri:Inspiration Biopharmaceuticals Inc: Research Funding. John:Inspiration Biopharmaceuticals Inc: Research Funding. Ramanan:Inspiration Biopharmaceuticals Inc: Research Funding. Liesner:Inspiration Biopharmaceuticals Inc: Research Funding. Shapiro:Inspiration Biopharmaceuticals Inc: Honoraria, Research Funding. Mills:Inspiration Biopharmaceuticals Inc: Employment. Lee:Inspiration Biopharmaceuticals Inc: Employment.
Author notes
Asterisk with author names denotes non-ASH members.
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