Summary of medicine characteristics - BYLVAY 1200 MICROGRAMS HARD CAPSULE
This medicinal product is subject to additional monitoring. This will allow quick identification of new safety information. Healthcare professionals are asked to report any suspected adverse reactions (see section 4.8) for how to report adverse reactions.
1 NAME OF THE MEDICINAL PRODUCT
Bylvay 1200 micrograms hard capsules
2 QUALITATIVE AND QUANTITATIVE COMPOSITION
Each hard capsule contains odevixibat sesquihydrate equivalent to
1 200 micrograms odevixibat
For the full list of excipients see section 6.1.
3 PHARMACEUTICAL FORM
Hard capsule
Size 3 capsule (15.9 mm x 5.82 mm) with orange opaque cap and body; imprinted “A1200” with black ink.
4 CLINICAL PARTICULARS
4.1 Therapeutic indications
Bylvay is indicated for the treatment of progressive familial intrahepatic cholestasis (PFIC) in patients aged 6 months or older (see sections 4.4 and 5.1).
4.2 Posology and method of administration
Treatment must be initiated and supervised by physicians experienced in the management of PFIC.
Posology
The recommended dose of odevixibat is 40 mcg/kg administered orally once daily in the morning. Odevixibat can be taken with or without food.
Table 1 shows the strength and number of capsules that should be administered daily based on body weight to approximate a 40 mcg/kg/day dose.
Table 1: Number of Bylvay capsules needed to achieve the nominal dose of
40 mcg/kg/day
Body weight (kg) | Number of 200 mcg capsules | Number of 400 mcg capsules | |
4 to < 7.5 | 1 | or | N/A |
7.5 to < 12.5 | 2 | or | 1 |
12.5 to < 17.5 | 3 | or | N/A |
17.5 to < 25.5 | 4 | or | 2 |
25.5 to < 35.5 | 6 | or | 3 |
35.5 to < 45.5 | 8 | or | 4 |
45.5 to < 55.5 | 10 | or | 5 |
> 55.5 | 12 | or | 6 |
Capsule strength/number in bold is recommended based on predicted ease of administration.
Dose escalation
Improvement in pruritus and reduction of serum bile acid levels may occur gradually in some patients after initiating odevixibat therapy. If an adequate clinical response has not been achieved after 3 months of continuous therapy, the dose may be increased to 120 mcg/kg/day (see section 4.4.).
Table 2 shows the strength and number of capsules that should be administered daily based on body weight to approximate a 120 mcg/kg/day dose, with a maximum daily dose of 7 200 mcg per day.
Table 2: Number of Bylvay capsules needed to achieve the nominal dose of
120 mcg/kg/day
Body weight (kg) | Number of 600 mcg capsules | Number of 1 200 mcg capsules | |
4 to < 7.5 | 1 | or | N/A |
7.5 to < 12.5 | 2 | or | 1 |
12.5 to < 17.5 | 3 | or | N/A |
17.5 to < 25.5 | 4 | or | 2 |
25.5 to < 35.5 | 6 | or | 3 |
35.5 to < 45.5 | 8 | or | 4 |
45.5 to < 55.5 | 10 | or | 5 |
> 55.5 | 12 | or | 6 |
Capsule strength/number in bold is recommended based on predicted ease of administration.
Alternative treatment should be considered in patients for whom no treatment benefit can be established following 6 months of continuous daily treatment with odevixibat.
Missed doses
If a dose of odevixibat is missed, the patient should take the forgotten dose as soon as possible without exceeding one dose per day.
Special populations
Renal impairment
No dose adjustment is required for patients with mild or moderate renal impairment.
There are no available clinical data for the use of odevixibat patients with moderate or severe renal impairment or end-stage renal disease (ESRD) requiring haemodialysis (see section 5.2).
Hepatic impairment
No dose adjustment is required for patients with mild or moderate hepatic impairment (see sections 5.1 and 5.2).
No data are available for PFIC patients with severe hepatic impairment (Child Pugh C). Additional monitoring for adverse reactions may be warranted in these patients when odevixibat is administered (see section 4.4).
Paediatric population
The safety and efficacy of odevixibat in children aged less than 6 months has not been established. No data are available.
Method of administration
Bylvay_is for oral use. To be taken with or without food in the morning (see section 5.2).
The larger 200 mcg and 600 mcg capsules are intended to be opened and sprinkled on food but may be swallowed whole.
The smaller 400 mcg and 1 200 mcg capsules are intended to be swallowed whole but may be opened and sprinkled on food.
If the capsule is to be swallowed whole, the patient should be instructed to take it with a glass of water in the morning.
For capsules to be opened, the patient should be instructed to:
place a small quantity (30 mL/2 tablespoons) of soft food (yoghurt, apple sauce, oatmeal porridge, banana puree, carrot puree, chocolate-flavoured pudding or rice pudding) in a bowl. The food should be at or below room temperature.
hold the capsule horizontally at both ends, twist in opposite directions and pull apart to empty the pellets into the bowl of soft food. The capsule should be gently tapped to ensure that all pellets will come out.
repeat the previous step if the dose requires more than one capsule.
gently mix the pellets with a spoon into the soft food.
administer the entire dose immediately after mixing. Do not store the mixture for future use.
drink a glass of water following the dose.
dispose all empty capsule shells.
4.3 Contraindications
Hypersensitivity to the active substance or to any of the excipients listed in section 6.1.
4.4 Special warnings and precautions for use
The mechanism of action of odevixibat requires that the enterohepatic circulation of bile acids and bile salt transport into biliary canaliculi is preserved. Conditions, medications or surgical procedures that impair either gastrointestinal motility, or enterohepatic circulation of bile acids, including bile salt transport to biliary canaliculi have the potential to reduce the efficacy of odevixibat. For this reason, e.g. patients with PFIC2 who have a complete absence or lack of function of Bile Salt Export Pump (BSEP) protein (i.e. patients with BSEP3 subtype of PFIC2) will not respond to odevixibat.
There are limited or no clinical data with odevixibat in PFIC subtypes other than 1 and 2.
Patients with severe hepatic impairment (Child-Pugh C) have not been studied (see section 5.2). Periodic liver function tests should be considered for patients with severe hepatic impairment.
Diarrhoea has been reported as a common adverse reaction when taking odevixibat. Diarrhoea may lead to dehydration. Patients should be monitored regularly to ensure adequate hydration during episodes of diarrhoea (see section 4.8).
In clinical trials, increased levels in liver function tests were observed in some patients receiving odevixibat. Assessment of liver function tests (alanine
aminotransferase, aspartate aminotransferase, gamma-glutamyl transferase, alkaline phosphatase and total bilirubin) is recommended for all patients prior to initiating Bylvay, with monitoring per standard clinical practice.
For patients with liver function test elevations, more frequent monitoring should be considered.
Assessment of fat-soluble vitamin levels (Vitamins A, D, E) and international normalised ratio (INR) are recommended for all patients prior to initiating Bylvay, with monitoring per standard clinical practice.
Treatment with odevixibat may impact the absorption of fat-soluble medicinal products, including lipophilic oral contraceptives (see sections 4.5 and 4.6).
4.5 Interaction with other medicinal products and other forms of interaction
Transporter-mediated interactions
Odevixibat is a substrate for the efflux transporter P-glycoprotein (P-gp). In adult healthy subjects, co-administration of the strong P-gp inhibitor itraconazole increased the plasma exposure of a single dose of odevixibat 7 200 mcg by approximately 50–60%. This increase is not considered clinically relevant. No other potentially relevant transporter-mediated interactions were identified in vitro (see section 5.2).
Cytochrome P450-mediated interactions
In vitro, odevixibat did not induce CYP enzymes (see section 5.2).
In in vitro studies, odevixibat was shown to be an inhibitor of CYP3A4/5 (see section 5.2).
In adult healthy subjects, concomitant use of odevixibat decreased the area under the curve (AUC) of oral midazolam (a CYP3A4 substrate) by 30% and 1-OH-midazolam exposure by less than 20%, which is not considered clinically relevant.
No interaction studies have been conducted with UDCA and rifampicin.
No interaction studies have been conducted with oral hormonal contraceptives or other lipophilic medicinal products. It cannot be excluded that the absorption of oral contraceptives is affected by concomitant use of odevixibat.
In clinical trials, decreased levels of fat-soluble vitamins were observed in some patients receiving odevixibat. Levels of fat-soluble vitamins should be monitored (see section 4.4).
Paediatric population
No interaction studies have been performed in paediatric patients. No differences are expected between the adult and paediatric populations.
4.6 Fertility, pregnancy and lactation
Women of childbearing potential
Women of childbearing potential should use an effective method of contraception when treated with Bylvay. Since the uptake of lipophilic oral contraceptives may be affected by odevixibat, a barrier contraceptive method should be used (see section 4.4).
Pregnancy
There are no or limited data from the use of odevixibat in pregnant women. Animal studies have shown reproductive toxicity (see section 5.3). Bylvay is not recommended during pregnancy and in women of childbearing potential not using contraception.
Breast-feeding
It is unknown whether odevixibat or its metabolites are excreted in human milk. There is insufficient information on the excretion of odevixibat in animal milk (see section 5.3).
A risk to newborns/infants cannot be excluded. A decision must be made whether to discontinue breast-feeding or to discontinue/abstain from Bylvay therapy, taking into account the benefit of breast-feeding for the child and the benefit of therapy for the mother.
Fertility
No fertility data are available in humans. Animal studies do not indicate any direct or indirect effects on fertility or reproduction (see section 5.3).
4.7 Effects on ability to drive and use machines
Bylvay has no or negligible influence on the ability to drive and use machines.
4.8 Undesirable effects
Summary of the safety profile
The most commonly reported adverse reaction was diarrhoea reported in (7%) of patients.
Tabulated list of adverse reactions
The table lists adverse reactions identified in clinical trials in patients with PFIC aged between 4 months to 25 years of age (median 3 years 7 months).
Adverse reactions are ranked according to system organ class, using the following convention: very common (> 1/10), common (> 1/100 to < 1/10), uncommon (> 1/1 000 to < 1/100), rare (> 1/10 000 to < 1/1 000), very rare (< 1/10 000) and not known (cannot be estimated from the available data).
Table 3:_____Frequency of adverse reactions in PFIC patients
MedDRA system organ class | Common |
Gastrointestinal disorders | diarrhoea, abdominal paina, diarrhoea haemorrhagic, faeces soft |
Hepatobiliary disorders | hepatomegaly |
aIncludes abdominal pain upper
Description of selected adverse reactions
Gastrointestinal adverse reactions
Gastrointestinal adverse reactions occurred at a frequency of 11% in patients treated with Bylvay. Adverse reactions of diarrhoea, abdominal pain and faeces soft were of short duration with most events < 5 days in duration; median time to first onset was 16 days. All reports were mild to moderate in severity and non-serious. Two patients experienced an adverse reaction of clinically significant diarrhoea defined as diarrhoea that persisted for 21 or more days without any other aetiology, was severe in intensity, required hospitalisation or was considered an important medical event, or presented with concurrent dehydration requiring treatment with oral or intravenous rehydration and/or other treatment intervention (see section 4.4). Treatment interruption was reported for diarrhoea in 4% of patients and discontinuation of Bylvay due to diarrhoea was reported in 1%.
Reporting of suspected adverse reactions
Reporting suspected adverse reactions after authorisation of the medicinal product is important. It allows continued monitoring of the benefit/risk balance of the medicinal product. Healthcare professionals are asked to report any suspected adverse reactions via the Yellow Card Scheme at: www.mhra.gov.uk/yellowcard or search for MHRA Yellow Card in the Google Play or Apple App Store.
4.9 Overdose
5 PHARMACOLOGICAL PROPERTIES
5.1 Pharmacodynamic properties
Pharmacotherapeutic group: Bile and liver therapy, other drugs for bile therapy, ATC code: A05AX05
Mechanism of action
Odevixibat is a reversible, potent, selective inhibitor of the ileal bile acid transporter (IBAT).
Pharmacodynamic effects
Odevixibat acts locally in the distal ileum to decrease the reuptake of bile acids and increase the clearance of bile acids through the colon, reducing the concentration of bile acids in the serum. The extent of reduction of serum bile acids does not correlate with systemic PK.
Clinical efficacy
The efficacy of Bylvay in patients with PFIC was evaluated in two phase 3 trials. Trial 1 was a 24-week, randomised, double-blind, placebo-controlled trial conducted in 62 patients with a confirmed diagnosis of PFIC Type 1 or Type 2. Patients were randomised 1:1:1 to placebo, or 40 or 120 mcg/kg/day odevixibat and stratified by PFIC Type (1 or 2) and age (6 months to 5 years, 6 to 12 years, and 13 to < 18 years). Patients with pathologic variations of the ABCB11 gene that predict complete absence of the BSEP protein and those with ALT > 10 x ULN or bilirubin > 10 x ULN were excluded. 13% of the patients had prior biliary diversion surgery. Patients completing Trial 1 were eligible to enrol in Trial 2, a 72-week open-label extension trial. The primary endpoint in Trial 1 was the proportion of patients with at least a 70% reduction in fasting serum bile acid levels or who achieved a level < 70 |imol/L at week 24.
The proportion of positive pruritus assessments at the patient level over the 24-week treatment period based on an observer-reported outcome (ObsRO) instrument was a secondary endpoint. A positive pruritus assessment was a score of < 1 or at least 1-point improvement from baseline. Pruritus assessments were conducted in the morning and evening using a 5-point scale (0–4). Additional secondary endpoints included changes from baseline to end of treatment in growth, sleep parameters (per ObsRO) and ALT.
Median (range) age of patients in Trial 1 was 3.2 (0.5 to 15.9) years; 50% were male and 84% were white. 27% of patients had PFIC Type 1 and 73% had PFIC Type 2. At baseline, 81% of patients were treated with UDCA, 66% with rifampicin, and 89% with UDCA and/or rifampicin. Baseline hepatic impairment per Child-Pugh classification was mild in 66% and moderate in 34% of patients. Baseline mean (SD) eGFR was 164 (30.6) mL/min/1.73 m2 Baseline mean (SD) ALT, AST and bilirubin levels were 99 (116.8) U/L, 101 (69.8) U/L, and 3.2 (3.57) mg/dL, respectively. Baseline mean (SD) pruritus score (range: 0–4) and serum bile acids levels were similar in odevixibat-treated patients (2.9 [0.089] and 252.1 [103.0] ^mol/L, respectively) and placebo-treated patients (3.0 [0.143] and 247.5 [101.1] |imol/L, respectively).
Table 4 presents the results of the comparison of the key efficacy results in Trial 1 between odevixibat and placebo. These data are displayed graphically over the 24-week treatment period in Figure 1 (serum bile acids) and Figure 2 (scratching scores).
Table 4: Comparison of key efficacy results for odevixibat vs.
placebo over the 24-week treatment period in patients with PFIC in trial 1
Efficacy endpoint | Placebo (N=20) | Odevixibat | ||
40 mcg/kg/day (N=23) | 120 mcg/kg/day (N=19) | Total (N=42) | ||
Proportion of patients with reduction in serum bile acids at end of treatment | ||||
n (%) | 0 (0.00, | 10 (43.5) | 4 (21.1) | 14 (33.3) |
(95% CI) | 16.84) | (23.19, 65.51) | (6.05, 45.57) | (19.57, 49.55) |
Difference in proportion vs. placebo (95% CI) | 0.44 (0.22, 0.66) | 0.21 (0.02, 0.46) | 0.33 (0.09, 0.50) | |
One-sided p-valuea | 0.0015 | 0.0174 | 0.0015 | |
Proportion of positive pruritus assessments over the treatment period | ||||
Proportion | 28.74 | 58.31 | 47.69 | 53.51 |
Difference in proportion (SE) vs. placebo (95% CI)b | 28.23 (9.18) (9.83, 46.64) | 21.71 (9.89) (1.87, 41.54) | 24.97 (8.24) (8.45, 41.49) |
aBased on Cochran Mantel Haenszel test stratified by PFIC Type. P-values for the dose groups are adjusted for multiplicity.
bBased on least squares means from an analysis of covariance model with daytime and night-time baseline pruritus scores as covariates and treatment group and stratification factors (PFIC Type and age category) as fixed effects.
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Weeks
Number of Patients
Placebo | 20 | 20 | 20 | 20 | 20 | 20 | 20 | 20 | 20 | 20 | 20 | 20 | 20 | 18 | 18 | 17 | 17 | 17 | 16 | 15 | 15 | 15 | 15 | 13 | 12 |
40 iig/kg/day | 23 | 23 | 23 | 23 | 23 | 23 | 23 | 22 | 22 | 23 | 23 | 23 | 23 | 19 | 19 | 19 | 19 | 20 | 19 | 18 | 19 | 19 | 19 | 19 | 17 |
120 ^g/kg/day | 19 | 19 | 19 | 19 | 19 | 19 | 19 | 19 | 19 | 18 | 18 | 18 | 18 | 16 | 16 | 16 | 16 | 16 | 16 | 16 | 16 | 16 | 16 | 15 | 14 |
All doses | 42 | 42 | 42 | 42 | 42 | 42 | 42 | 41 | 41 | 41 | 41 | 41 | 41 | 35 | 35 | 35 | 35 | 36 | 35 | 34 | 35 | 35 | 35 | 34 | 31 |
In line with the results for reduction of pruritus (scratching), odevixibat reduced the percentage of days the patient required soothing, and patients less often required help falling asleep and had fewer days needing to sleep with a caregiver. Treatment with odevixibat also led to improvements from baseline in liver function test results (Table 5). The effect of odevixibat on growth parameters over 24 weeks is also presented.
Table 5: Comparison of efficacy results for growth and hepatic biochemical parameters for odevixibat vs. placebo over the 24-week treatment period in patients with PFIC in trial 1
Efficacy endpoint | Placebo (N=20) | Odevixibat | ||
40 mcg/kg/day | 120 mcg/kg/day | Total |
(N=23) | (N=19) | (N=42) | ||
Alanine aminotransferase (U/L) (mean [SE]) | ||||
Baseline | 76.9 (12.57) | 127.7 (34.57) | 89.1 (19.95) | 110.2 (20.96) |
Change to Week 24 | 3.7 (4.95) | –27.9 (17.97) | –25.3 (22.47) | –26.7 (13.98) |
Mean difference vs. placebo (95% CI)a | –14.8 (16.63) (-48.3, 18.7) | –14.9 (17.25) (-49.6, 19.9) | –14.8 (15.05) (-45.1, 15.4) | |
Aspartate aminotransferase (U/L) (mean [SE]) | ||||
Baseline | 90.2 (11.59) | 114.2 (17.24) | 96.0 (16.13) | 106.0 (11.87) |
Change to Week 24 | 4.7 (5.84) | –36.7 (12.21) | –27.0 (19.42) | –32.1 (11.02) |
Total bilirubin (iimol/L) (mean [SE]) | ||||
Baseline | 53.3 (12.97) | 52.2 (10.13) | 57.0 (18.05) | 54.4 (9.75) |
Change to Week 24 | –9.6 (15.16) | –23.7 (9.23) | –19.3 (13.62) | –21.7 (7.92) |
Height z-scores (mean [SE]) | ||||
Baseline | –2.26 (0.34) | –1.45 (0.27) | –2.09 (0.37) | –1.74 (0.23) |
Change to Week 24 | –0.16 (0.10) | 0.05 (0.11) | 0.00 (0.16) | 0.03 (0.09) |
Mean difference vs. placebo (95% CI)a | 0.32 (0.16) (0.00, 0.65) | 0.15 (0.17) (-0.18, 0.48) | 0.24 (0.14) (-0.05, 0.53) | |
Weight z-scores (mean [SE]) | ||||
Baseline | –1.52 (0.32) | –0.74 (0.27) | –1.19 (0.35) | –0.94 (0.21) |
Change to Week 24 | 0.10 (0.10) | 0.29 (0.11) | 0.15 (0.12) | 0.22 (0.08) |
Mean difference vs. placebo (95% CI)a | 0.28 (0.14) (-0.01, 0.57) | 0.08 (0.15) (-0.22, 0.37) | 0.18 (0.13) (-0.08, 0.44) | |
aBased on least squares means from a mixed | model for repeated measures |
(MMRM) with baseline value as a covariate, and treatment group, visit, treatment-by-visit interaction, treatment-by-baseline interaction and stratification factors (PFIC type and age category) as fixed effects.
Trial 2 is an interim cut of data from an ongoing 72-week open-label extension trial in PFIC patients treated with Bylvay 120 mcg/kg/day. The 79 patients (PFIC1 [22%], PFIC2 [51%], PFIC3 [5%] or PFIC6 [1%]) treated with 120 mcg/kg/day for up to 48 weeks experienced a durable effect on serum bile acids reduction, improvement in pruritus score, ALT, AST and total bilirubin. Across the 79 patients, 45 had assessments on or after 48 weeks of treatment with odevixibat, including 13, 30, 1 and 1 patients with PFIC1, PFIC2, PFIC3, and PFIC6, respectively; 9, 21, 4, and 0 patients, respectively, had not reached 48 weeks of treatment and were ongoing at the data cut-off. Overall, 7 patients with PFIC2 had discontinued prior to 48 weeks of treatment with odevixibat. Improvements in z-scores for height and weight indicate an enhanced growth velocity and the potential for catch-up growth in actively growing children.
Paediatric population
The European Medicines Agency has deferred the obligation to submit the results of studies with Bylvay in paediatric population less than 6 months; see section 4.2 for information on paediatric use.
Exceptional circumstances
This medicinal product has been authorised under ‘Exceptional
Circumstances’. This means that due to the rarity of the disease it has not been possible to obtain complete information on this medicinal product. The European Medicines Agency will review any new information which may become available every year and this SmPC will be updated as necessary.
5.2 Pharmacokinetic properties
Absorption
Odevixibat is minimally absorbed following oral administration; absolute bioavailability data in humans are not available, and estimated relative bioavailability is < 1%. Peak odevixibat plasma concentration (Cmax) is reached within 1 to 5 hours. Simulated Cmax values in a paediatric PFIC patient population for the 40 and 120 mcg/kg/day doses are 0.211 ng/mL and 0.623 ng/mL, respectively, and AUC values were 2.26 ng x h/mL and 5.99 ng x h/mL, respectively. There is minimal accumulation of odevixibat following once-daily dosing.
Effect of food
Systemic exposure of odevixibat does not predict efficacy. Therefore, no dose adjustment for food effects is considered necessary. Concomitant administration of a high-fat meal (800 – 1 000 calories with approximately 50% of total caloric content of the meal from fat) resulted in decreases of approximately 72% and 62% in Cmax and AUC0–24, respectively, compared to administration under fasted conditions. When odevixibat was sprinkled on apple sauce, decreases of approximately 39% and 36% in Cmax and AUC0–24, respectively, were observed compared to administration under fasted conditions. Taking into account the lack of PK/PD relationship and need for sprinkling the odevixibat capsule contents on food for younger children, odevixibat can be administered with food.
Distribution
Odevixibat is more than 99% bound to human plasma proteins. The mean body weight adjusted apparent volumes of distribution (V/F) in paediatric patients for the 40 and 120 mcg/kg/day dose regimens are 40.3 and 43.7 L/kg, respectively.
Biotransformation
Odevixibat is minimally metabolised in humans.
Elimination
Following administration of a single oral dose of 3 000 mcg of radiolabeled odevixibat in healthy adults, the average percent recovery of the administered dose was 82.9% in faeces; less than 0.002% was recovered in the urine. More than 97% of faecal radioactivity was determined to be unchanged odevixibat.
The mean body weight normalised apparent total clearances CL/F in paediatric patients for the 40 and 120 mcg/kg/day dose regimens are 26.4 and 23.0 L/kg/h, respectively, and the mean half-life is approximately 2.5 hours.
Linearity/non-linearity
The Cmax and AUC0-t increase with increasing doses in a dose-proportional manner; however due to the high interindividual variability of approximately 40%, it is not possible to estimate the dose proportionality accurately.
Pharmacokinetic/pharmacodynamic relationship(s)
Consistent with the mechanism and site of action of odevixibat in the gastrointestinal tract no relationship between systemic exposure and clinical effects is observed. Also, no dose-response relationship could be established for the investigated dose range 10–200 mcg/kg/day and the PD parameters C4 and FGF19.
Special populations
No clinically significant differences in the pharmacokinetics of odevixibat were observed based on age, sex or race.
Hepatic impairment
The majority of patients with PFIC presented with some degree of hepatic impairment because of the disease. Hepatic metabolism of odevixibat is not a major component of the elimination of odevixibat. Analysis of data from a placebo-controlled study in patients with PFIC Types 1 and 2 did not demonstrate a clinically important impact of mildly impaired hepatic function (Child Pugh A) on the pharmacokinetics of odevixibat. Although, body weight adjusted CL/F values were lower and body weight adjusted V/F values were larger in paediatric patients with PFIC with Child Pugh B compared to healthy subjects, the safety profile was comparable between the patient groups. Patients with severe hepatic impairment (Child-Pugh C) have not been studied.
Renal impairment
There are no clinical data in patients with renal impairment, but the impact of renal impairment is expected to be small due to low systemic exposure and odevixibat is not excreted in urine.
In vitro studies
In in vitro studies, odevixibat did not inhibit CYPs 1A2, 2B6, 2C8, 2C9, 2C19 or 2D6 at clinically relevant concentrations, but was shown to be an inhibitor of CYP3A4/5.
Odevixibat does not inhibit the transporters P-gp, breast cancer resistance protein (BCRP), organic anion transporter (OATP1B1, OATP1B3, OAT1, OAT3), organic cation transporter (OCT2), multidrug and toxin extrusion transporter (MATE1 or MATE2-K).
Odevixibat is not a BCRP substrate.
5.3 Preclinical safety data
6 PHARMACEUTICAL PARTICULARS
6.1 List of excipients
Microcrystalline cellulose
Hypromellose Ph.Eur
Capsule shell
Hypromellose
Titanium dioxide (E171)
Yellow iron oxide (E172)
Red iron oxide (E172)
Printing ink
Shellac Ph.Eur
Propylene glycol
Black iron oxide (E172)
6.2 Incompatibilities
Not applicable.
6.3 Shelf life
2 years
6.4 Special precautions for storage
Store in the original package in order to protect from light. This medicinal product does not require any special temperature storage conditions.
6.5 Nature and contents of container
High-density polyethylene (HDPE) bottle with a tamper evident, child resistant polypropylene closure.
Pack size: 30 hard capsules
6.6 Special precautions for disposal
6.6 Special precautions for disposalAny unused medicinal product or waste material should be disposed of in accordance with local requirements.
7 MARKETING AUTHORISATION HOLDER
Albireo AB
Arvid Wallgrens backe 20
413 46 Göteborg
Sweden
8 MARKETING AUTHORISATION NUMBER(S)
PLGB 36216/0004
9 DATE OF FIRST AUTHORISATION/RENEWAL OF THE AUTHORISATION
07/09/2021