даклинза

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Overdose

There is limited experience of accidental overdose of daclatasvir in clinical studies. In phase 1 clinical studies, healthy subjects who received up to 100 mg once daily for up to 14 days or single doses up to 200 mg had no unexpected adverse reactions.

There is no known antidote for overdose of daclatasvir. Treatment of overdose with daclatasvir should consist of general supportive measures, including monitoring of vital signs, and observation of the patient's clinical status. Because daclatasvir is highly protein bound (99%) and has a molecular weight >500, dialysis is unlikely to significantly reduce plasma concentrations of daclatasvir.

Contraindications

Coadministration with medicinal products that strongly induce cytochrome P450 3A4 (CYP3A4) and P-glycoprotein transporter (P-gp) and thus may lead to lower exposure and loss of efficacy of Даклинза. These active substances include but are not limited to phenytoin, carbamazepine, oxcarbazepine, phenobarbital, rifampicin, rifabutin, rifapentine, systemic dexamethasone, and the herbal product St John's wort (Hypericum perforatum).

Incompatibilities

Not applicable.

Pharmaceutical form

Film-coated tablet

Undesirable effects

Summary of the safety profile

The overall safety profile of daclatasvir is based on data from 2215 patients with chronic HCV infection who received Даклинза once daily either in combination with sofosbuvir with or without ribavirin (n=679, pooled data) or in combination with peginterferon alfa and ribavirin (n=1536, pooled data) from a total of 14 clinical studies.

Даклинза in combination with sofosbuvir

The most frequently reported adverse reactions were fatigue, headache, and nausea. Grade 3 adverse reactions were reported in less than 1% of patients, and no patients had a Grade 4 adverse reaction. Four patients discontinued the Даклинза regimen for adverse events, only one of which was considered related to study therapy.

Даклинза in combination with peginterferon alfa and ribavirin

The most frequently reported adverse reactions were fatigue, headache, pruritus, anaemia, influenza-like illness, nausea, insomnia, neutropenia, asthenia, rash, decreased appetite, dry skin, alopecia, pyrexia, myalgia, irritability, cough, diarrhoea, dyspnoea and arthralgia. The most frequently reported adverse reactions of at least Grade 3 severity (frequency of 1% or greater) were neutropenia, anaemia, lymphopenia and thrombocytopenia. The safety profile of daclatasvir in combination with peginterferon alfa and ribavirin was similar to that seen with peginterferon alfa and ribavirin alone, including among patients with cirrhosis.

Tabulated list of adverse reactions

Adverse reactions are listed in Table 5 by regimen, system organ class and frequency: 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) and very rare (<1/10,000). Within each frequency grouping, adverse reactions are presented in order of decreasing seriousness.

Table 5: Adverse reactions in clinical studies

System Organ Class

Adverse Reactions

Frequency

Даклинза +sofosbuvir + ribavirin

N=203

Даклинза +sofosbuvir

N=476

Blood and lymphatic system disorders

very common

anaemia

Metabolism and nutrition disorders

common

decreased appetite

Psychiatric disorders

common

insomnia, irritability

insomnia

Nervous system disorders

very common

headache

headache

common

dizziness, migraine

dizziness, migraine

Vascular disorders

common

hot flush

Respiratory, thoracic and mediastinal disorders

common

dyspnoea, dyspnoea exertional, cough, nasal congestion

Gastrointestinal disorders

very common

nausea

common

diarrhoea, vomiting, abdominal pain, gastrooesophageal reflux disease, constipation, dry mouth, flatulence

nausea, diarrhoea, abdominal pain

Skin and subcutaneous tissue disorders

common

rash, alopecia, pruritus, dry skin

Musculoskeletal and connective tissue disorders

common

arthralgia, myalgia

arthralgia, myalgia

General disorders and administration site conditions

very common

fatigue

fatigue

Laboratory abnormalities

In clinical studies of Даклинза in combination with sofosbuvir with or without ribavirin, 2% of patients had Grade 3 haemoglobin decreases; all of these patients received Даклинза + sofosbuvir + ribavirin. Grade 3/4 increases in total bilirubin were observed in 5% of patients (all in patients with HIV co-infection who were receiving concomitant atazanavir, with Child-Pugh A, B, or C cirrhosis, or who were post-liver transplant).

Description of selected adverse reactions

Cardiac arrhythmias

Cases of severe bradycardia and heart block have been observed when Даклинза is used in combination with sofosbuvir and concomitant amiodarone and/or other drugs that lower heart rate.

Paediatric population

The safety and efficacy of Даклинза in children and adolescents aged <18 years have not yet been established. No data are available.

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.

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Preclinical safety data

Toxicology

In repeat-dose toxicology studies in animals, hepatic effects (Kupffer-cell hypertrophy/ hyperplasia, mononuclear cell infiltrates and bile duct hyperplasia) and adrenal gland effects (changes in cytoplasmic vacuolation and adrenal cortical hypertrophy/hyperplasia) were observed at exposures similar or slightly higher than the clinical AUC exposure. In dogs, bone marrow hypocellularity with correlating clinical pathology changes were observed at exposures 9-fold the clinical AUC exposure. None of these effects have been observed in humans.

Carcinogenesis and mutagenesis

Daclatasvir was not carcinogenic in mice or in rats at exposures 8-fold or 4-fold, respectively, the clinical AUC exposure. No evidence of mutagenic or clastogenic activity was observed in in vitro mutagenesis (Ames) tests, mammalian mutation assays in Chinese hamster ovary cells, or in an in vivo oral micronucleus study in rats.

Fertility

Daclatasvir had no effects on fertility in female rats at any dose tested. The highest AUC value in unaffected females was 18-fold the clinical AUC exposure. In male rats, effects on reproductive endpoints were limited to reduced prostate/seminal vesicle weights, and minimally increased dysmorphic sperm at 200 mg/kg/day; however, neither finding adversely affected fertility or the number of viable conceptuses sired. The AUC associated with this dose in males is 19-fold the clinical AUC exposure.

Embryo-foetal development

Daclatasvir is embryotoxic and teratogenic in rats and rabbits at exposures at or above 4-fold (rat) and 16-fold (rabbit) the clinical AUC exposure. Developmental toxicity consisted of increased embryofoetal lethality, reduced foetal body weights and increased incidence of foetal malformations and variations. In rats, malformations mainly affected the brain, skull, eyes, ears, nose, lip, palate or limbs and in rabbits, the ribs and cardiovascular area. Maternal toxicity including mortality, abortions, adverse clinical signs, decreases in body weight and food consumption was noted in both species at exposures 25-fold (rat) and 72-fold (rabbit) the clinical AUC exposure.

In a study of pre- and postnatal development in rats, there was neither maternal nor developmental toxicity at doses up to 50 mg/kg/day, associated with AUC values 2-fold the clinical AUC exposure. At the highest dose (100 mg/kg/day), maternal toxicity included mortality and dystocia; developmental toxicity included slight reductions in offspring viability in the peri- and neonatal periods; and reductions in birth weight that persisted into adulthood. The AUC value associated with this dose is 4-fold the clinical AUC exposure.

Excretion into milk

Daclatasvir was excreted into the milk of lactating rats with concentrations 1.7- to 2-fold maternal plasma levels.

Therapeutic indications

Даклинза is indicated in combination with other medicinal products for the treatment of chronic hepatitis C virus (HCV) infection in adults.

1.

Pharmacotherapeutic group

Direct-acting antiviral, ATC code: J05AX14

Pharmacodynamic properties

Pharmacotherapeutic group: Direct-acting antiviral, ATC code: J05AX14

Mechanism of action

Daclatasvir is an inhibitor of nonstructural protein 5A (NS5A), a multifunctional protein that is an essential component of the HCV replication complex. Daclatasvir inhibits both viral RNA replication and virion assembly.

Antiviral activity in cell culture

Daclatasvir is an inhibitor of HCV genotypes 1a and 1b replication in cell-based replicon assays with effective concentration (50% reduction, EC50) values of 0.003-0.050 and 0.001-0.009 nM, respectively, depending on the assay method. The daclatasvir EC50 values in the replicon system were 0.003-1.25 nM for genotypes 3a, 4a, 5a and 6a, and 0.034-19 nM for genotype 2a as well as 0.020 nM for infectious genotype 2a (JFH-1) virus.

Daclatasvir showed additive to synergistic interactions with interferon alfa, HCV nonstructural protein 3 (NS3) PIs, HCV nonstructural protein 5B (NS5B) non-nucleoside inhibitors, and HCV NS5B nucleoside analogues in combination studies using the cell-based HCV replicon system. No antagonism of antiviral activity was observed.

No clinically relevant antiviral activity was observed against a variety of RNA and DNA viruses, including HIV, confirming that daclatasvir, which inhibits a HCV-specific target, is highly selective for HCV.

Resistance in cell culture

Substitutions conferring daclatasvir resistance in genotypes 1-4 were observed in the N-terminal 100 amino acid region of NS5A in a cell-based replicon system. L31V and Y93H were frequently observed resistance substitutions in genotype 1b, while M28T, L31V/M, Q30E/H/R, and Y93C/H/N were frequently observed resistance substitutions in genotype 1a. These substitutions conferred low level resistance (EC50 <1 nM) for genotype 1b, and higher levels of resistance for genotype 1a (EC50 up to 350 nM). The most resistant variants with single amino acid substitution in genotype 2a and genotype 3a were F28S (EC50 >300 nM) and Y93H (EC50 >1,000 nM), respectively. In genotype 4, amino acid substitutions at 30 and 93 (EC50 < 16 nM) were frequently selected.

Cross-resistance

HCV replicons expressing daclatasvir-associated resistance substitutions remained fully sensitive to interferon alfa and other anti-HCV agents with different mechanisms of action, such as NS3 protease and NS5B polymerase (nucleoside and non-nucleoside) inhibitors.

Clinical efficacy and safety

In clinical studies of daclatasvir in combination with sofosbuvir or with peginterferon alfa and ribavirin, plasma HCV RNA values were measured using the COBAS TaqMan HCV test (version 2.0), for use with the High Pure System, with a lower limit of quantification (LLOQ) of 25 IU/ ml. SVR was the primary endpoint to determine the HCV cure rate, which was defined as HCV RNA less than LLOQ at 12 weeks after the end of treatment (SVR12) for studies AI444040, ALLY-1 (AI444215), ALLY-2 (AI444216), ALLY-3 (AI444218), AI444042 and AI444043 and as HCV RNA undetectable at 24 weeks after the end of treatment (SVR24) for study AI444010.

Daclatasvir in combination with sofosbuvir

The efficacy and safety of daclatasvir 60 mg once daily in combination with sofosbuvir 400 mg once daily in the treatment of patients with chronic HCV infection were evaluated in four open-label studies (AI444040, ALLY-1, ALLY-2 and ALLY-3).

In study AI444040, 211 adults with HCV genotype 1, 2, or 3 infection and without cirrhosis received daclatasvir and sofosbuvir, with or without ribavirin. Among the 167 patients with HCV genotype 1 infection, 126 were treatment-naïve and 41 had failed prior therapy with a PI regimen (boceprevir or telaprevir). All 44 patients with HCV genotype 2 (n=26) or 3 (n=18) infection were treatment-naïve. Treatment duration was 12 weeks for 82 treatment-naïve HCV genotype 1 patients, and 24 weeks for all other patients in the study. The 211 patients had a median age of 54 years (range: 20 to 70); 83% were white; 12% were black/African-American; 2% were Asian; 20% were Hispanic or Latino. The mean score on the FibroTest (a validated non-invasive diagnostic assay) was 0.460 (range: 0.03 to 0.89). Conversion of the FibroTest score to the corresponding METAVIR score suggests that 35% of all patients (49% of patients with prior PI failure, 30% of patients with genotype 2 or 3) had >F3 liver fibrosis. Most patients (71%, including 98% of prior PI failures) had IL-28B rs12979860 non-CC genotypes.

SVR12 was achieved by 99% patients with HCV genotype 1, 96% of those with genotype 2 and 89% of those with genotype 3 (see Tables 6 and 7). Response was rapid (viral load at Week 4 showed that more than 97% of patients responded to therapy), and was not influenced by HCV subtype (1a/1b), IL28B genotype, or use of ribavirin. Among treatment-naïve patients with HCV RNA results at both follow-up Weeks 12 and 24, concordance between SVR12 and SVR24 was 99.5% independent of treatment duration.

Treatment-naïve patients with HCV genotype 1 who received 12 weeks of treatment had a similar response as those treated for 24 weeks (Table 6).

Table 6: Treatment outcomes, daclatasvir in combination with sofosbuvir, HCV genotype 1 in Study AI444040

Treatment-naïve

Prior telaprevir or boceprevir failures

daclatasvir + sofosbuvir

N=70

daclatasvir + sofosbuvir + ribavirin

N=56

All

N=126

daclatasvir + sofosbuvir

N=21

daclatasvir + sofosbuvir + ribavirin

N=20

All

N=41

End of treatment

HCV RNA undetectable

70 (100%)

56 (100%)

126 (100%)

19 (91%)

19 (95%)

38 (93%)

SVR12 (overall)*

70 (100%)

55 (98%)*

125 (99%)*

21 (100%)

20 (100%)

41 (100%)

12 weeks treatment duration

41/41 (100%)

40/41 (98%)

81/82 (99%)

--

--

--

24 weeks treatment duration

29/29 (100%)

15/15 (100%)

44/44 (100%)

21 (100%)

20 (100%)

41 (100%)

> F3 liver fibrosis

--

--

41/41 (100%)

--

--

20/20 (100%)

* Patients who had missing data at follow-up Week 12 were considered responders if their next available HCV RNA value was <LLOQ. One treatment-naïve patient was missing both post-treatment Weeks 12 and 24 data.

Table 7: Treatment outcomes, daclatasvir in combination with sofosbuvir for 24 weeks, treatment-naïve patients with HCV genotype 2 or 3 in Study AI444040

Genotype 2

Genotype 3

daclatasvir + sofosbuvir

N=17

daclatasvir + sofosbuvir + ribavirin

N=9

All Genotype 2

N=26

daclatasvir + sofosbuvir

N=13

daclatasvir + sofosbuvir + ribavirin

N=5

All Genotype 3

N=18

End of treatment

HCV RNA undetectable

17 (100%)

9 (100%)

26 (100%)

11 (85%)

5 (100%)

16 (89%)

SVR12*

17 (100%)

8 (89%)*

25 (96%)*

11 (85%)

5 (100%)

16 (89%)

> F3 liver fibrosis

8/8 (100%)

5/5 (100%)

Virologic failure

Virologic breakthrough**

0

0

0

1 (8%)

0

1 (6%)

Relapse**

0

0

0

1/11 (9%)

0

1/16 (6%)

* Patients who had missing data at follow-up Week 12 were considered responders if their next available HCV RNA value was <LLOQ. One patient with HCV genotype 2 infection was missing both post-treatment Week 12 and 24 data.

** The patient with virologic breakthrough met the original protocol definition of confirmed HCV RNA <LLOQ, detectable at treatment Week 8. Relapse was defined as HCV RNA >LLOQ during follow-up after HCV RNA <LLOQ at end of treatment. Relapse includes observations through follow-up Week 24.

Advanced cirrhosis and post-liver transplant (ALLY-1)

In study ALLY-1, the regimen of daclatasvir, sofosbuvir, and ribavirin administered for 12 weeks was evaluated in 113 adults with chronic hepatitis C and Child-Pugh A, B or C cirrhosis (n=60) or HCV recurrence after liver transplantation (n=53). Patients with HCV genotype 1, 2, 3, 4, 5 or 6 infection were eligible to enroll. Patients received daclatasvir 60 mg once daily, sofosbuvir 400 mg once daily, and ribavirin (600 mg starting dose) for 12 weeks and were monitored for 24 weeks post treatment. Patients demographics and main disease characteristics are summarised in Table 8.

Table 8: Demographics and main disease characteristics in Study ALLY-1

Cirrhotic cohort

N = 60

Post-Liver Transplant

N = 53

Age (years): median (range)

58 (19-75)

59 (22-82)

Race: White

57 (95%)

51 (96%)

Black/African American

3 (5%)

1 (2%)

Other

0

1 (2%)

HCV genotype:

1a

 

34 (57%)

 

31 (58%)

1b

11 (18%)

10 (19%)

2

5 (8%)

0

3

6 (10%)

11 (21%)

4

4 (7%)

0

6

0

1 (2%)

Fibrosis stage

F0

0

6 (11%)

F1

1 (2%)

10 (19%)

F2

3 (5%)

7 (13%)

F3

8 (13%)

13 (25%)

F4

48 (80%)

16 (30%)

Not reported

0

1 (2%)

CP classes

ND

CP A

12 (20%)

CP B

32 (53%)

CP C

16 (27%)

MELD score

ND

mean

13.3

median

13.0

Q1, Q3

10, 16

Min, Max

8, 27

ND: Not determined

SVR12 was achieved by 83% (50/60) of patients in the cirrhosis cohort, with a marked difference between patients with Child-Pugh A or B (92-94%) as compared to those with Child-Pugh C and 94% of patients in the post-liver transplant cohort (Table 9). SVR rates were comparable regardless of age, race, gender, IL28B allele status, or baseline HCV RNA level. In the cirrhosis cohort, 4 patients with hepatocellular carcinoma underwent liver transplantation after 1-71 days of treatment; 3 of the 4 patients received 12 weeks of post-liver transplant treatment extension and 1 patient, treated for 23 days before transplantation, did not receive treatment extension. All 4 patients achieved SVR12.

Table 9: Treatment outcomes, daclatasvir in combination with sofosbuvir and ribavirin for 12 weeks, patients with cirrhosis or HCV recurrence after liver transplantation, Study ALLY-1

Cirrhotic cohort

N=60

Post-LiverTransplant

N=53

End of treatment

HCV RNA undetectable

58/60 (97%)

53/53 (100%)

SVR12

Relapse

SVR12

Relapse

All patients

50/60 (83%)

9/58* (16%)

50/53 (94%)

3/53 (6%)

Cirrhosis

ND

ND

CP A

11/12 (92%)

1/12 (8%)

CP B

30/32 (94%)

2/32 (6%)

CP C

9/16 (56%)

6/14 (43%)

Genotype 1

37/45 (82%)

7/45 (16%)

39/41 (95%)

2/41 (5%)

1a

26/34 (77%)

7/33 (21%)

30/31 (97%)

1/31 (3%)

1b

11/11 (100%)

0%

9/10 (90%)

1/10 (10%)

Genotype 2

4/5 (80%)

1/5 (20%)

--

--

Genotype 3

5/6 (83%)

1/6 (17%)

10/11 (91%)

1/11 (9%)

Genotype 4

4/4 (100%)

0%

--

--

Genotype 6

--

--

1/1 (100%)

0%

ND: Not determined

* 2 patients had detectable HCV RNA at end of treatment; 1 of these patients achieved SVR.

HCV/HIV co-infection (ALLY-2)

In study ALLY-2, the combination of daclatasvir and sofosbuvir administered for 12 weeks was evaluated in 153 adults with chronic hepatitis C and HIV co-infection; 101 patients were HCV treatment-naïve and 52 patients had failed prior HCV therapy. Patients with HCV genotype 1, 2, 3, 4, 5, or 6 infection were eligible to enroll, including patients with compenstated cirrhosis (Child-Pugh A). The dose of daclatasvir was adjusted for concomitant antiretroviral use. Patient demographics and baseline disease characteristics are summarised in Table 10.

Table 10: Demographics and baseline characteristics in Study ALLY-2

Patient disposition

daclatasvir + sofosbuvir

12 weeks

N = 153

Age (years): median (range)

53 (24-71)

Race:

White

97 (63%)

Black/African American

50 (33%)

Other

6 (4%)

HCV genotype:

1a

 

104 (68%)

1b

23 (15%)

2

13 (8%)

3

10 (7%)

4

3 (2%)

Compensated cirrhosis

24 (16%)

Concomitant HIV therapy:

PI-based

 

70 (46%)

NNRTI-based

40 (26%)

Other

41 (27%)

None

2 (1%)

Overall, SVR12 was achieved by 97% (149/153) of patients administered daclatasvir and sofosbuvir for 12 weeks in ALLY-2. SVR rates were >94% across combination antiretroviral therapy (cART) regimens, including boosted-PI-, NNRTI-, and integrase inhibitor (INSTI)-based therapies.

SVR rates were comparable regardless of HIV regimen, age, race, gender, IL28B allele status, or baseline HCV RNA level. Outcomes by prior treatment experience are presented in Table 11.

A third treatment group in study ALLY-2 included 50 HCV treatment-naïve HIV co-infected patients who received daclatasvir and sofosbuvir for 8 weeks. Demographic and baseline characteristics of these 50 patients were generally comparable to those for patients who received 12 weeks of study treatment. The SVR rate for patients treated for 8 weeks was lower with this treatment duration as summarized in Table 11.

Table 11: Treatment outcomes, daclatasvir in combination with sofosbuvir in patients with HCV/HIV co-infection in Study ALLY-2

8 weeks therapy

12 weeks therapy

HCV Treatment-naïve

N=50

HCV Treatment-naïve

N=101

HCV Treatment-experienced*

N=52

End of treatment

HCV RNA undetectable

50/50 (100%)

100/101 (99%)

52/52 (100%)

SVR12

38/50 (76%)

98/101 (97%)

51/52 (98%)

No cirrhosis**

34/44 (77%)

88/90 (98%)

34/34 (100%)

With cirrhosis**

3/5 (60%)

8/9 (89%)

14/15 (93%)

Genotype 1

31/41 (76%)

80/83 (96%)

43/44 (98%)

1a

1b

28/35 (80%)

3/6 (50%)

68/71 (96%)

12/12 (100%)

32/33 (97%)

11/11 (100%)

Genotype 2

5/6 (83%)

11/11 (100%)

2/2 (100%)

Genotype 3

2/3 (67%)

6/6 (100%)

4/4 (100%)

Genotype 4

0

1/1 (100%)

2/2 (100%)

Virologic failure

Detectable HCV RNA at end of treatment

0

1/101 (1%)

0

Relapse

10/50 (20%)

1/100 (1%)

1/52 (2%)

Missing post-treatment data

2/50 (4%)

1/101 (1%)

0

* Mainly interferon-based therapy +/-NS3/4 PI.

** Cirrhosis was determined by liver biopsy, FibroScan >14.6 kPa, or FibroTest score >0.75 and aspartate aminotransferase (AST): platelet ratio index (APRI) >2. For 5 patients, cirrhosis status was indeterminate.

HCV Genotype 3 (ALLY-3)

In study ALLY-3, the combination of daclatasvir and sofosbuvir administered for 12 weeks was evaluated in 152 adults infected with HCV genotype 3; 101 patients were treatment-naïve and 51 patients had failed prior antiviral therapy. Median age was 55 years (range: 24 to 73); 90% of patients were white; 4% were black/African-American; 5% were Asian; 16% were Hispanic or Latino. The median viral load was 6.42 log10 IU/ml, and 21% of patients had compensated cirrhosis. Most patients (61%) had IL-28B rs12979860 non-CC genotypes.

SVR12 was achieved in 90% of treatment-naïve patients and 86% of treatment-experienced patients. Response was rapid (viral load at Week 4 showed that more than 95% of patients responded to therapy) and was not influenced by IL28B genotype. SVR12 rates were lower among patients with cirrhosis (see Table 12).

Table 12: Treatment outcomes, daclatasvir in combination with sofosbuvir for 12 weeks, patients with HCV genotype 3 in Study ALLY-3

Treatment-naïve

N=101

Treatment-experienced*

N=51

Total

N=152

End of treatment

HCV RNA undetectable

100 (99%)

51 (100%)

151 (99%)

SVR12

91 (90%)

44 (86%)

135 (89%)

No cirrhosis**

73/75 (97%)

32/34 (94%)

105/109 (96%)

With cirrhosis**

11/19 (58%)

9/13 (69%)

20/32 (63%)

Virologic failure

Virologic breakthrough

0

0

0

Detectable HCV RNA at end of treatment

1 (1%)

0

1 (0.7%)

Pharmacokinetic properties

The pharmacokinetic properties of daclatasvir were evaluated in healthy adult subjects and in patients with chronic HCV. Following multiple oral doses of daclatasvir 60 mg once daily in combination with peginterferon alfa and ribavirin in treatment-naïve patients with genotype 1 chronic HCV, the geometric mean (CV%) daclatasvir Cmax was 1534 (58) ng/ml, AUC0-24h was 14122 (70) ng-h/ml, and Cmin was 232 (83) ng/ml.

Absorption

Daclatasvir administered as a tablet was readily absorbed following multiple oral doses with peak plasma concentrations occurring between 1 and 2 hours.

Daclatasvir Cmax, AUC, and Cmin increased in a near dose-proportional manner. Steady state was achieved after 4 days of once-daily administration. At the 60 mg dose, exposure to daclatasvir was similar between healthy subjects and HCV-infected patients.

In vitro and in vivo studies showed that daclatasvir is a substrate of P-gp. The absolute bioavailability of the tablet formulation is 67%.

Effect of food on oral absorption

In healthy subjects, administration of daclatasvir 60 mg tablet after a high-fat meal decreased daclatasvir Cmax and AUC by 28% and 23%, respectively, compared with administration under fasting conditions. Administration of daclatasvir 60 mg tablet after a light meal resulted in no reduction in daclatasvir exposure.

Distribution

At steady state, protein binding of daclatasvir in HCV-infected patients was approximately 99% and independent of dose at the dose range studied (1 mg to 100 mg). In patients who received daclatasvir 60 mg tablet orally followed by 100 μg [13C,15N]-daclatasvir intravenous dose, estimated volume of distribution at steady state was 47 l. In vitro studies indicate that daclatasvir is actively and passively transported into hepatocytes. The active transport is mediated by OCT1 and other unidentified uptake transporters, but not by organic anion transporter (OAT) 2, sodium-taurocholate cotransporting polypeptide (NTCP), or OATPs.

Daclatasvir is an inhibitor of P-gp, OATP 1B1 and BCRP. In vitro daclatasvir is an inhibitor of renal uptake transporters, OAT1 and 3, and OCT2, but is not expected to have a clinical effect on the pharmacokinetics of substrates of these transporters.

Biotransformation

In vitro and in vivo studies demonstrate that daclatasvir is a substrate of CYP3A, with CYP3A4 being the major CYP isoform responsible for the metabolism. No metabolites circulated at levels more than 5% of the parent concentration. Daclatasvir in vitro did not inhibit (IC50 >40 µM) CYP enzymes 1A2, 2B6, 2C8, 2C9, 2C19, or 2D6.

Elimination

Following single-dose oral administration of 14C-daclatasvir in healthy subjects, 88% of total radioactivity was recovered in feces (53% as unchanged drug) and 6.6% was excreted in the urine (primarily as unchanged drug). These data indicate that the liver is the major clearance organ for daclatasvir in humans. In vitro studies indicate that daclatasvir is actively and passively transported into hepatocytes. The active transport is mediated by OCT1 and other unidentified uptake transporters. Following multiple-dose administration of daclatasvir in HCV-infected patients, the terminal elimination half-life of daclatasvir ranged from 12 to 15 hours. In patients who received daclatasvir 60 mg tablet orally followed by 100 μg [13C,15N]-daclatasvir intravenous dose, the total clearance was 4.24 l/h.

Special populations

Renal impairment

The pharmacokinetics of daclatasvir following a single 60 mg oral dose were studied in non-HCV infected subjects with renal impairment. Daclatasvir unbound AUC was estimated to be 18%, 39% and 51% higher for subjects with creatinine clearance (CLcr) values of 60, 30 and 15 ml/min, respectively, relative to subjects with normal renal function. Subjects with end-stage renal disease requiring haemodialysis had a 27% increase in daclatasvir AUC and a 20% increase in unbound AUC compared to subjects with normal renal function.

Hepatic impairment

The pharmacokinetics of daclatasvir following a single 30 mg oral dose were studied in non-HCV infected subjects with mild (Child-Pugh A), moderate (Child-Pugh B), and severe (Child-Pugh C) hepatic impairment compared with unimpaired subjects. The Cmax and AUC of total daclatasvir (free and protein-bound drug) were lower in subjects with hepatic impairment; however, hepatic impairment did not have a clinically significant effect on the free drug concentrations of daclatasvir.

Elderly

Population pharmacokinetic analysis of data from clinical studies indicated that age had no apparent effect on the pharmacokinetics of daclatasvir.

Paediatric population

The pharmacokinetics of daclatasvir in paediatric patients have not been evaluated.

Gender

Population pharmacokinetic analysis identified gender as a statistically significant covariate on daclatasvir apparent oral clearance (CL/F) with female subjects having slightly lower CL/F, but the magnitude of the effect on daclatasvir exposure is not clinically important.

Race

Population pharmacokinetic analysis of data from clinical studies identified race (categories “other” [patients who are not white, black or Asian] and “black”) as a statistically significant covariate on daclatasvir apparent oral clearance (CL/F) and apparent volume of distribution (Vc/F) resulting in slightly higher exposures compared to white patients, but the magnitude of the effect on daclatasvir exposure is not clinically important.

Name of the medicinal product

Даклинза

Qualitative and quantitative composition

Daclatasvir

Special warnings and precautions for use

Даклинза must not be administered as monotherapy. Даклинза must be administered in combination with other medicinal products for the treatment of chronic HCV infection.

Severe bradycardia and heart block

Cases of severe bradycardia and heart block have been observed when Даклинза is used in combination with sofosbuvir and concomitant amiodarone with or without other drugs that lower heart rate. The mechanism is not established.

The concomitant use of amiodarone was limited through the clinical development of sofosbuvir plus direct-acting antivirals (DAAs). Cases are potentially life threatening, therefore amiodarone should only be used in patients on Даклинза and sofosbuvir when other alternative antiarrhythmic treatments are not tolerated or are contraindicated.

Should concomitant use of amiodarone be considered necessary it is recommended that patients are closely monitored when initiating Даклинза in combination with sofosbuvir. Patients who are identified as being at high risk of bradyarrhythmia should be continuously monitored for 48 hours in an appropriate clinical setting.

Due to the long half-life of amiodarone, appropriate monitoring should also be carried out for patients who have discontinued amiodarone within the past few months and are to be initiated on Даклинза in combination with sofosbuvir.

All patients receiving Даклинза and sofosbuvir in combination with amiodarone with or without other drugs that lower heart rate should also be warned of the symptoms of bradycardia and heart block and should be advised to seek medical advice urgently should they experience them.

Genotype-specific activity

Data to support the treatment of genotype 2 infection with Даклинза and sofosbuvir are limited.

Data from study ALLY-3 (AI444218) support a 12-week treatment duration of Даклинза + sofosbuvir for treatment-naïve and -experienced patients with genotype 3 infection without cirrhosis. Lower rates of SVR were observed for patients with cirrhosis. Data from compassionate use programmes which included patients with genotype 3 infection and cirrhosis, support the use of Даклинза + sofosbuvir for 24 weeks in these patients. The relevance of adding ribavirin to that regimen is unclear.

The clinical data to support the use of Даклинза and sofosbuvir in patients infected with HCV genotypes 4 and 6 are limited. There are no clinical data in patients with genotype 5.

Patients with Child-Pugh C liver disease

The safety and efficacy of Даклинза in the treatment of HCV infection in patients with Child-Pugh C liver disease have been established in the clinical study ALLY-1 (AI444215, Даклинза + sofosbuvir + ribavirin for 12 weeks); however, SVR rates were lower than in patients with Child-Pugh A and B. Therefore, a conservative treatment regimen of Даклинза + sofosbuvir +/- ribavirin for 24 weeks is proposed for patients with Child-Pugh C. Ribavirin may be added based on clinical assessment of an individual patient.

HCV/HBV (hepatitis B virus) co-infection

Cases of hepatitis B virus (HBV) reactivation, some of them fatal, have been reported during or after treatment with direct-acting antiviral agents. HBV screening should be performed in all patients before initiation of treatment. HBV/HCV co-infected patients are at risk of HBV reactivation, and should therefore be monitored and managed according to current clinical guidelines.

Retreatment with daclatasvir

The efficacy of Даклинза as part of a retreatment regimen in patients with prior exposure to a NS5A inhibitor has not been established.

Pregnancy and contraception requirements

Даклинза should not be used during pregnancy or in women of childbearing potential not using contraception. Use of highly effective contraception should be continued for 5 weeks after completion of Даклинза therapy.

When Даклинза is used in combination with ribavirin, the contraindications and warnings for that medicinal product are applicable. Significant teratogenic and/or embryocidal effects have been demonstrated in all animal species exposed to ribavirin; therefore, extreme care must be taken to avoid pregnancy in female patients and in female partners of male patients (see the Summary of Product Characteristics for ribavirin).

Interactions with medicinal products

Coadministration of Даклинза can alter the concentration of other medicinal products and other medicinal products may alter the concentration of daclatasvir.-drug interactions.

Paediatric population

Даклинза is not recommended for use in children and adolescents aged below 18 years because the safety and efficacy have not been established in this population.

Important information about some of the ingredients in Даклинза

Даклинза contains lactose. Patients with rare hereditary problems of galactose intolerance, the Lapp lactase deficiency or glucose-galactose malabsorption should not take this medicine.

Effects on ability to drive and use machines

Dizziness has been reported during treatment with Даклинза in combination with sofosbuvir, and dizziness, disturbance in attention, blurred vision and reduced visual acuity have been reported during treatment with Даклинза in combination with peginterferon alfa and ribavirin.

Dosage (Posology) and method of administration

Treatment with Даклинза should be initiated and monitored by a physician experienced in the management of chronic hepatitis C.

Posology

The recommended dose of Даклинза is 60 mg once daily, to be taken orally with or without meals.

Даклинза must be administered in combination with other medicinal products. The Summary of Product Characteristics for the other medicinal products in the regimen should also be consulted before initiation of therapy with Даклинза.

Table 1: Recommended treatment for Даклинза interferon-free combination therapy

Patient population*

Regimen and duration

HCV GT 1 or 4

Patients without cirrhosis

Даклинза + sofosbuvir for 12 weeks

Patients with cirrhosis

CP A or B

 

Даклинза + sofosbuvir + ribavirin for 12 weeks

or

Даклинза + sofosbuvir (without ribavirin) for 24 weeks

CP C

Даклинза + sofosbuvir +/- ribavirin for 24 weeks

HCV GT 3

Patients without cirrhosis

Даклинза + sofosbuvir for 12 weeks

Patients with cirrhosis

Даклинза + sofosbuvir +/- ribavirin for 24 weeks

Recurrent HCV infection post-liver transplant (GT 1, 3 or 4)

Patients without cirrhosis

Даклинза + sofosbuvir + ribavirin for 12 weeks

Patients with CP A or B cirrhosis

GT 1 or 4

GT 3

 

Даклинза + sofosbuvir + ribavirin for 12 weeks

Даклинза + sofosbuvir +/- ribavirin for 24 weeks

Patients with CP C cirrhosis

Даклинза + sofosbuvir +/- ribavirin for 24 weeks

GT: Genotype; CP: Child Pugh

* Includes patients co-infected with human immunodeficiency virus (HIV).

Даклинза + peginterferon alfa + ribavirin

This regimen is an alternative recommended regimen for patients with genotype 4 infection, without cirrhosis or with compensated cirrhosis. Даклинза is given for 24 weeks, in combination with 24-48 weeks of peginterferon alfa and ribavirin:

- If HCV RNA is undetectable at both treatment weeks 4 and 12, all 3 components of the regimen should be continued for a total duration of 24 weeks.

- If undetectable HCV RNA is achieved, but not at both treatment weeks 4 and 12, Даклинза should be discontinued at 24 weeks and peginterferon alfa and ribavirin continued for a total duration of 48 weeks.

Ribavirin Dosing Guidelines

The dose of ribavirin, when combined with Даклинза, is weight-based (1,000 or 1,200 mg in patients <75 kg or >75 kg, respectively). Refer to the Summary of Product Characteristics of ribavirin.

For patients with Child-Pugh A, B, or C cirrhosis or recurrence of HCV infection after liver transplantation, the recommended initial dose of ribavirin is 600 mg daily with food. If the starting dose is well-tolerated, the dose can be titrated up to a maximum of 1,000-1,200 mg daily (breakpoint 75 kg). If the starting dose is not well-tolerated, the dose should be reduced as clinically indicated, based on haemoglobin and creatinine clearance measurements (see Table 2).

Table 2: Ribavirin dosing guidelines for coadministration with Даклинза regimen for patients with cirrhosis or post-transplant

Laboratory Value/Clinical Criteria

Ribavirin Dosing Guideline

Haemoglobin

>12 g/dL

600 mg daily

> 10 to ≤12 g/dL

400 mg daily

> 8.5 to ≤10 g/dL

200 mg daily

≤8.5 g/dL

Discontinue ribavirin

Creatinine Clearance

>50 mL/min

Follow guidelines above for haemoglobin

>30 to ≤50 mL/min

200 mg every other day

≤30 mL/min or haemodialysis

Discontinue ribavirin

Dose modification, interruption and discontinuation

Dose modification of Даклинза to manage adverse reactions is not recommended. If treatment interruption of components in the regimen is necessary because of adverse reactions, Даклинза must not be given as monotherapy.

There are no virologic treatment stopping rules that apply to the combination of Даклинза with sofosbuvir.

Treatment discontinuation in patients with inadequate on-treatment virologic response during treatment with Даклинза, peginterferon alfa and ribavirin

It is unlikely that patients with inadequate on-treatment virologic response will achieve a sustained virologic response (SVR); therefore discontinuation of treatment is recommended in these patients. The HCV RNA thresholds that trigger discontinuation of treatment (i.e. treatment stopping rules) are presented in Table 3.

Table 3: Treatment stopping rules in patients receiving Даклинза in combination with peginterferon alfa and ribavirin with inadequate on-treatment virologic response

HCV RNA

Action

Treatment week 4: >1000 IU/ml

Discontinue Даклинза, peginterferon alfa and ribavirin

Treatment week 12: >25 IU/ml

Discontinue Даклинза, peginterferon alfa and ribavirin

Treatment week 24: >25 IU/ml

Discontinue peginterferon alfa and ribavirin (treatment with Даклинза is complete at week 24)

Dose recommendation for concomitant medicines

Strong inhibitors of cytochrome P450 enzyme 3A4 (CYP3A4)

The dose of Даклинза should be reduced to 30 mg once daily when coadministered with strong inhibitors of CYP3A4.

Moderate inducers of CYP3A4

The dose of Даклинза should be increased to 90 mg once daily when coadministered with moderate inducers of CYP3A4.

Missed doses

Patients should be instructed that, if they miss a dose of Даклинза, the dose should be taken as soon as possible if remembered within 20 hours of the scheduled dose time. However, if the missed dose is remembered more than 20 hours after the scheduled dose, the dose should be skipped and the next dose taken at the appropriate time.

Special populations

Elderly

No dose adjustment of Даклинза is required for patients aged >65 years.

Renal impairment

No dose adjustment of Даклинза is required for patients with any degree of renal impairment.

Hepatic impairment

No dose adjustment of Даклинза is required for patients with mild (Child-Pugh A, score 5-6), moderate (Child-Pugh B, score 7-9) or severe (Child-Pugh C, score >10) hepatic impairment.

Paediatric population

The safety and efficacy of Даклинза in children and adolescents aged below 18 years have not yet been established. No data are available.

Method of administration

Даклинза is to be taken orally with or without meals. Patients should be instructed to swallow the tablet whole. The film-coated tablet should not be chewed or crushed due the unpleasant taste of the active substance.

Special precautions for disposal and other handling

Any unused medicinal product or waste material should be disposed of in accordance with local requirements.