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Dimethyl Fumarate 120 mg gastro-resistant hard capsules

Active Ingredient:
dimethyl fumarate
Company:  
Genus Pharmaceuticals See contact details
ATC code: 
L04AX07
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About Medicine
{healthcare_pro_orange} This information is for use by healthcare professionals
Last updated on emc: 07 May 2024
1. Name of the medicinal product

Dimethyl Fumarate 120 mg gastro-resistant hard capsules

2. Qualitative and quantitative composition

Each gastro-resistant hard capsule contains 120 mg dimethyl fumarate

For the full list of excipients, see section 6.1.

3. Pharmaceutical form

Gastro-resistant hard capsule

Green opaque cap and white opaque body, capsule shell size No. 0 printed in black ink with “ DMF 120” on the body containing white to off-white minitablets.

4. Clinical particulars

4.1 Therapeutic indications

Dimethyl Fumarate is indicated for the treatment of adult patients with relapsing remitting multiple sclerosis (see section 5.1 for important information on the populations for which efficacy has been established).

4.2 Posology and method of administration

Treatment should be initiated under supervision of a physician experienced in the treatment of multiple sclerosis.

Posology

The starting dose is 120 mg twice a day. After 7 days, the dose should be increased to the recommended maintenance dose of 240 mg twice a day (see section 4.4).

If a patient misses a dose, a double dose should not be taken. The patient may take the missed dose only if they leave 4 hours between doses. Otherwise, the patient should wait until the next scheduled dose.

Temporary dose reduction to 120 mg twice a day may reduce the occurrence of flushing and gastrointestinal adverse reactions. Within 1 month, the recommended maintenance dose of 240 mg twice a day should be resumed. Dimethyl Fumarate should be taken with food (see section 5.2). For those patients who may experience flushing or gastrointestinal adverse reactions, taking Dimethyl Fumarate with food may improve tolerability (see sections 4.4, 4.5 and 4.8).

Special populations

Elderly

Clinical studies of Dimethyl Fumarate had limited exposure to patients aged 55 years and above, and did not include sufficient numbers of patients aged 65 and over to determine whether they respond differently than younger patients (see section 5.2). Based on the mode of action of the active substance there are no theoretical reasons for any requirement for dose adjustments in the elderly.

Renal and hepatic impairment

Dimethyl Fumarate has not been studied in patients with renal or hepatic impairment. Based on clinical pharmacology studies, no dose adjustments are needed (see section 5.2). Caution should be used when treating patients with severe renal or severe hepatic impairment (see section 4.4).

Method of administration

For oral use.

The capsule should be swallowed whole. The capsule or its contents should not be crushed, divided, dissolved, sucked or chewed as the enteric-coating of the microtablets prevents irritant effects on the gut.

4.3 Contraindications

Hypersensitivity to the active substance or to any of the excipients listed in section 6.1. Suspected or confirmed Progressive Multifocal Leukoencephalopathy (PML)

4.4 Special warnings and precautions for use

Blood/laboratory tests

Changes in renal laboratory tests have been seen in clinical trials in subjects treated with dimethyl fumarate (see section 4.8). The clinical implications of these changes are unknown. Assessment of renal function (e.g., creatinine, blood urea nitrogen and urinalysis) is recommended prior to treatment initiation, after 3 and 6 months of treatment, every 6 to 12 months thereafter and as clinically indicated.

Drug-induced liver injury, including liver enzyme increase (≥ 3 upper limit of normal (ULN)) and elevation of total bilirubin levels (≥ 2 ULN) can result from treatment with dimethyl fumarate. The time to onset can be directly, several weeks or longer. Resolution of the adverse reactions has been observed after treatment was discontinued. Assessment of serum aminotransferases (e.g., alanine aminotransferase (ALT), aspartate aminotransferase (AST)) and total bilirubin levels are recommended prior to treatment initiation and during treatment as clinically indicated. Patients treated with Dimethyl Fumarate may develop lymphopenia (see section 4.8). Prior to initiating treatment with Dimethyl Fumarate, a current complete blood count, including lymphocytes, must be performed.

If lymphocyte count is found to be below the normal range, thorough assessment of possible causes should be completed prior to initiation of treatment with Dimethyl Fumarate. Dimethyl fumarate has not been studied in patients with pre-existing low lymphocyte counts and caution should be exercised when treating these patients. Dimethyl Fumarate should not be initiated in patients with severe lymphopenia (lymphocyte counts <0.5 x 109/l).

After starting therapy, complete blood counts, including lymphocytes, must be performed every 3 months.

Enhanced vigilance due to an increased risk for Progressive Multifocal Leukoencephalopathy (PML) is recommended in patients with lymphopenia as follows:

• Dimethyl Fumarate should be discontinued in patients with prolonged severe lymphopenia (lymphocyte counts <0.5 x 109/l) persisting for more than 6 months.

• In patients with sustained moderate reductions of absolute lymphocyte counts ≥ 0.5 x 109 /l and < 0.8 x 109 /l for more than six months, the benefit/risk of Dimethyl Fumarate treatment should be re-assessed.

• In patients with lymphocyte counts below lower limit of normal (LLN) as defined by local laboratory reference range, regular monitoring of absolute lymphocyte counts is recommended. Additional factors that might further augment the individual PML risk should be considered (see subsection on PML below).

Lymphocyte counts should be followed until recovery. Upon recovery and in the absence of alternative treatment options, decisions about whether or not to restart Dimethyl Fumarate after treatment discontinuation should be based on clinical judgement

Magnetic Resonance imaging (MRI)

Before initiating treatment with Dimethyl Fumarate, a baseline MRI should be available (usually within 3 months) as a reference. The need for further MRI scanning should be considered in accordance with national and local recommendations. MRI imaging may be considered as part of increased vigilance in patients considered at increased risk of PML. In case of clinical suspicion of PML, MRI should be performed immediately for diagnostic purposes.

Progressive Multifocal Leukoencephalopathy (PML)

PML has been reported in patients treated with Dimethyl Fumarate (see section 4.8). PML is an opportunistic infection caused by John-Cunningham virus (JCV), which may be fatal or result in severe disability. PML cases have occurred with dimethyl fumarate and other medicinal products containing fumarates in the setting of lymphopenia (lymphocyte counts below LLN). Prolonged moderate to severe lymphopenia appears to increase the risk of PML with Dimethyl Fumarate, however, risk cannot be excluded in patients with mild lymphopenia. Additional factors that might contribute to an increased risk for PML in the setting of lymphopenia are:

- duration of Dimethyl Fumarate therapy. Cases of PML have occurred after approximately1 to 5 years of treatment, although the exact relationship with duration of treatment is unknown.

- profound decreases in CD4+ and especially in CD8+ T cell counts, which are important for immunological defence (see section 4.8), and - prior immunosuppressive or immunomodulatory therapy (see below).

Physicians should evaluate their patients to determine if the symptoms are indicative of neurological dysfunction and, if so, whether these symptoms are typical of MS or possibly suggestive of PML.

At the first sign or symptom suggestive of PML, Dimethyl Fumarate should be withheld and appropriate diagnostic evaluations, including determination of JCV DNA in cerebrospinal fluid (CSF) by quantitative polymerase chain reaction (PCR) methodology, need to be performed. The symptoms of PML may be similar to an MS relapse. Typical symptoms associated with PML are diverse, progress over days to weeks, and include progressive weakness on one side of the body or clumsiness of limbs, disturbance of vision, and changes in thinking, memory, and orientation leading to confusion and personality changes. Physicians should be particularly alert to symptoms suggestive of PML that the patient may not notice. Patients should also be advised to inform their partner or caregivers about their treatment, since they may notice symptoms that the patient is not aware of.

PML can only occur in the presence of a JCV infection. It should be considered that the influence of lymphopenia on the accuracy of serum antiJCV antibody testing has not been studied in dimethyl fumarate treated patients. It should also be noted that a negative anti-JCV antibody test (in the presence of normal lymphocyte counts) does not preclude the possibility of subsequent JCV infection.

If a patient develops PML, Dimethyl Fumarate must be permanently discontinued.

Prior treatment with immunosuppressive or immunomodulating therapies

No studies have been performed evaluating the efficacy and safety of Dimethyl Fumarate when switching patients from other disease modifying therapies to Dimethyl Fumarate. The contribution of prior immunosuppressive therapy to the development of PML in dimethyl fumarate treated patients is possible.

PML cases have occurred in patients who had previously been treated with natalizumab, for which PML is an established risk. Physicians should be aware that cases of PML occurring following recent discontinuation of natalizumab may not have lymphopenia.

In addition, a majority of confirmed PML cases with Dimethyl Fumarate occurred in patients with prior immunomodulatory treatment.

When switching patients from another disease modifying therapy to Dimethyl Fumarate, the half-life and mode of action of the other therapy should be considered in order to avoid an additive immune effect while at the same time, reducing the risk of reactivation of MS. A complete blood count is recommended prior to initiating Dimethyl Fumarate and regularly during treatment (see Blood/laboratory tests above).

Severe renal and hepatic impairment

Dimethyl Fumarate has not been studied in patients with severe renal or severe hepatic impairment and caution should, therefore, be used in these patients (see section 4.2).

Severe active gastrointestinal disease

Dimethyl Fumarate has not been studied in patients with severe active gastrointestinal disease and caution should, therefore, be used in these patients.

Flushing

In clinical trials, 34% of Dimethyl Fumarate treated patients experienced flushing. In the majority of patients who experienced flushing, it was mild or moderate in severity. Data from healthy volunteer studies suggest that dimethyl fumarate-associated flushing is likely to be prostaglandin mediated. A short course of treatment with 75 mg non-enteric coated acetylsalicylic acid may be beneficial in patients affected by intolerable flushing (see section 4.5). In two healthy volunteer studies, the occurrence and severity of flushing over the dosing period was reduced.

In clinical trials, 3 patients out of a total of 2,560 patients treated with dimethyl fumarate experienced serious flushing symptoms that were probable hypersensitivity or anaphylactoid reactions. These events were not lifethreatening, but led to hospitalisation. Prescribers and patients should be alert to this possibility in the event of severe flushing reactions (see sections 4.2, 4.5 and 4.8).

Anaphylactic reactions

Cases of anaphylaxis/anaphylactoid reaction have been reported following Dimethyl Fumarate administration in the post-marketing setting. Symptoms may include dyspnoea, hypoxia, hypotension, angioedema, rash or urticaria.

The mechanism of dimethyl fumarate induced anaphylaxis is unknown. Reactions generally occur after the first dose, but may also occur at any time during treatment, and may be serious and life threatening. Patients should be instructed to discontinue Dimethyl Fumarate and seek immediate medical care if they experience signs or symptoms of anaphylaxis. Treatment should not be restarted (see section 4.8).

Infections

In phase III placebo-controlled studies, the incidence of infections (60% vs 58%) and serious infections (2% vs 2%) was similar in patients treated with Dimethyl Fumarate or placebo, respectively. However, due to Dimethyl Fumarate immunomodulatory properties (see section 5.1), if a patient develops a serious infection, suspending treatment with Dimethyl Fumarate should be considered and the benefits and risks should be reassessed prior to re-initiation of therapy. Patients receiving Dimethyl Fumarate should be instructed to report symptoms of infections to a physician. Patients with serious infections should not start treatment with Dimethyl Fumarate until the infection(s) is resolved.

There was no increased incidence of serious infections observed in patients with lymphocyte counts <0.8x109/l or <0.5x109/l (see Section 4.8). If therapy is continued in the presence of moderate to severe prolonged lymphopenia, the risk of an opportunistic infection, including PML, cannot be ruled out (see section 4.4 subsection PML).

Herpes zoster infections

Cases of herpes zoster have occurred with Dimethyl Fumarate. The majority of cases were non-serious, however, serious cases, including disseminated herpes zoster, herpes zoster ophthalmicus, herpes zoster oticus, herpes zoster infection neurological, herpes zoster meningoencephalitis and herpes zoster meningomyelitis have been reported. These events may occur at any time during treatment. Monitor patients taking Dimethyl Fumarate for signs and symptoms of herpes zoster especially when concurrent lymphocytopenia is reported. If herpes zoster occurs, appropriate treatment for herpes zoster should be administered. Consider withholding Dimethyl Fumarate treatment in patients with serious infections until the infection has resolved (see section 4.8).

Treatment initiation

Dimethyl Fumarate treatment should be started gradually to reduce the occurrence of flushing and gastrointestinal adverse reactions (see section 4.2).

Fanconi syndrome

Cases of Fanconi syndrome have been reported for a medicinal product containing dimethyl fumarate in combination with other fumaric acid esters. Early diagnosis of Fanconi syndrome and discontinuation of dimethyl fumarate treatment are important to prevent the onset of renal impairment and osteomalacia, as the syndrome is usually reversible. The most important signs are: proteinuria, glucosuria (with normal blood sugar levels), hyperaminoaciduria and phosphaturia (possibly concurrent with hypophosphatemia). Progression might involve symptoms such as polyuria, polydipsia and proximal muscle weakness. In rare cases hypophosphataemic osteomalacia with non-localised bone pain, elevated alkaline phosphatase in serum and stress fractures may occur. Importantly, Fanconi syndrome can occur without elevated creatinine levels or low glomerular filtration rate. In case of unclear symptoms Fanconi syndrome should be considered and appropriate examinations should be performed.

Paediatric population

The safety profile is qualitatively similar in paediatric patients compared to adults and therefore the warnings and precautions also apply to the paediatric patients. For quantitative differences in the safety profile see section 4.8. The long-term safety of Dimethyl Fumarate in paediatric population has not yet been established.

4.5 Interaction with other medicinal products and other forms of interaction

Dimethyl Fumarate has not been studied in combination with anti-neoplastic or immunosuppressive therapies and caution should, therefore, be used during concomitant administration. In multiple sclerosis clinical studies, the concomitant treatment of relapses with a short course of intravenous corticosteroids was not associated with a clinically relevant increase of infection.

Concomitant administration of non-live vaccines according to national vaccination schedules may be considered during Dimethyl Fumarate therapy. In a clinical study involving a total of 71 patients with relapsing remitting multiple sclerosis, patients on Dimethyl Fumarate 240 mg twice daily for at least 6 months (n=38) or non-pegylated interferon for at least 3 months (n=33), mounted a comparable immune response (defined as ≥ 2-fold increase from pre- to post-vaccination titer) to tetanus toxoid (recall antigen) and a conjugated meningococcal C polysaccharide vaccine (neoantigen), while the immune response to different serotypes of an unconjugated 23-valent pneumococcal polysaccharide vaccine (T-cell independent antigen) varied in both treatment groups. A positive immune response defined as a ≥ 4-fold increase in antibody titer to the three vaccines, was achieved by fewer subjects in both treatment groups. Small numerical differences in the response to tetanus toxoid and pneumococcal serotype 3 polysaccharide were noted in favour of non-pegylated interferon.

No clinical data are available on the efficacy and safety of live attenuated vaccines in patients taking Dimethyl Fumarate. Live vaccines might carry an increased risk of clinical infection and should not be given to patients treated with Dimethyl Fumarate unless, in exceptional cases, this potential risk is considered to be outweighed by the risk to the individual of not vaccinating.

During treatment with Dimethyl Fumarate, simultaneous use of other fumaric acid derivatives (topical or systemic) should be avoided.

In humans, dimethyl fumarate is extensively metabolised by esterases before it reaches the systemic circulation and further metabolism occurs through the tricarboxylic acid cycle, with no involvement of the cytochrome P450 (CYP) system. Potential drug interaction risks were not identified from in vitro CYP-inhibition and induction studies, a p-glycoprotein study, or studies of the protein binding of dimethyl fumarate and monomethyl fumarate (a primary metabolite of dimethyl fumarate).

Commonly used medicinal products in patients with multiple sclerosis, intramuscular interferon beta-1a and glatiramer acetate, were clinically tested for potential interactions with dimethyl fumarate and did not alter the pharmacokinetic profile of dimethyl fumarate.

Evidence from healthy volunteer studies suggests that Dimethyl Fumarate-associated flushing is likely to be prostaglandin mediated. In two healthy volunteer studies, the administration of 325 mg (or equivalent) non-enteric coated acetylsalicylic acid, 30 minutes prior to Dimethyl Fumarate, dosing over 4 days and over 4 weeks, respectively, did not alter the pharmacokinetic profile of Dimethyl Fumarate. Potential risks associated with acetylsalicylic acid therapy should be considered prior to co-administration with Dimethyl Fumarate in patients with Relapsing Remitting MS. Long term (> 4 weeks) continuous use of acetylsalicylic acid has not been studied (see sections 4.4 and 4.8).

Concurrent therapy with nephrotoxic medicinal products (such as aminoglycosides, diuretics, non-steroidal anti-inflammatory drugs or lithium) may increase the potential of renal adverse reactions (e.g., proteinuria see section 4.8) in patients taking Dimethyl Fumarate (see section 4.4 Blood/laboratory tests).

Consumption of moderate amounts of alcohol did not alter exposure to dimethyl fumarate and was not associated with an increase in adverse reactions. Consumption of large quantities of strong alcoholic drinks (more than 30% alcohol by volume) should be avoided within an hour of taking Dimethyl Fumarate, as alcohol may lead to increased frequency of gastrointestinal adverse reactions.

In vitro CYP induction studies did not demonstrate an interaction between Dimethyl Fumarate and oral contraceptives. In an in vivo study, co-administration of Dimethyl Fumarate with a combined oral contraceptive (norgestimate and ethinyl estradiol) did not elicit any relevant change in oral contraceptive exposure. No interaction studies have been performed with oral contraceptives containing other progestogens, however an effect of Dimethyl Fumarate on their exposure is not expected.

Paediatric population

Interaction studies have only been performed in adults.

4.6 Fertility, pregnancy and lactation

Pregnancy

There are no or limited amount of data from the use of dimethyl fumarate in pregnant women. Animal studies have shown reproductive toxicity (see section 5.3). Dimethyl Fumarate is not recommended during pregnancy and in women of childbearing potential not using appropriate contraception (see section 4.5). Dimethyl Fumarate should be used during pregnancy only if clearly needed and if the potential benefit justifies the potential risk to the foetus

Breast-feeding

It is unknown whether dimethyl fumarate or its metabolites are excreted in human milk. A risk to the newborns/infants cannot be excluded. A decision must be made whether to discontinue breast-feeding or to discontinue Dimethyl Fumarate therapy. The benefit of breast-feeding for the child and the benefit of therapy for the woman should be taken into account.

Fertility

There are no data on the effects of dimethyl fumarate on human fertility. Data from preclinical studies do not suggest that dimethyl fumarate would be associated with an increased risk of reduced fertility (see section 5.3).

4.7 Effects on ability to drive and use machines

Dimethyl Fumarate has no or negligible influence on the ability to drive and use machines. No studies on the ability to drive and use machines have been conducted but no effects potentially influencing this ability were found to be related to dimethyl fumarate in clinical studies.

4.8 Undesirable effects

Summary of the safety profile

The most common adverse reactions (incidence ≥ 10%) for patients treated with dimethyl fumarate were flushing and gastrointestinal events (i.e., diarrhoea, nausea, abdominal pain, abdominal pain upper). Flushing and gastrointestinal events tend to begin early in the course of treatment (primarily during the first month) and in patients who experience flushing and gastrointestinal events, these events may continue to occur intermittently throughout treatment with Dimethyl Fumarate. The most commonly reported adverse reactions leading to discontinuation (incidence >1%) in patients treated with Dimethyl Fumarate were flushing (3%) and gastrointestinal events (4%).

In placebo-controlled and uncontrolled clinical studies, a total of 2,468 patients have received Dimethyl Fumarate and been followed for periods up to 4 years with an overall exposure equivalent to 3,588 person-years. Approximately 1,056 patients have received more than 2 years of treatment with Dimethyl Fumarate. The experience in uncontrolled clinical trials is consistent with the experience in the placebo-controlled clinical trials.

Tabulated summary of adverse reactions

Adverse reactions arising from clinical studies, post-authorisation safety studies and spontaneous reports, are presented in the table below. The adverse reactions are presented as MedDRA preferred terms under the MedDRA System Organ Class. The incidence of the adverse reactions below are expressed according to the following categories:

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)

Not known

(frequency cannot be estimated from the available data)

Table 1: Adverse reactions identified in controlled clinical trials and postmarketing

MedDRA System Organ

Class Adverse reaction

Frequency category

Infections and infestations

Gastroenteritis

Common

Progressive multifocal leukoencephalopathy (PML)

Not known

Herpes zoster

Not known

Blood and lymphatic system disorders

Lymphopenia

Common

Leucopenia

Common

Thrombocytopenia

Uncommon

Immune system disorders

Hypersensitivity

Uncommon

Anaphylaxis

Not known

Dyspnoea

Not known

Hypoxia

Not known

Hypotension

Not known

Angioedema

Not known

Nervous system disorders

Burning sensation

Common

Vascular disorders

Flushing

Very common

Hot flush

Common

Respiratory, thoracic and mediastinal disorders

Rhinorrhoea

Not known

Gastrointestinal disorders

Diarrhoea

Very common

Nausea

Very common

Abdominal pain upper

Very common

Abdominal pain

Very common

Vomiting

Common

Dyspepsia

Common

Gastritis

Common

Gastrointestinal disorder

Common

Hepatobiliary disorders

Aspartate aminotransferase increased

Common

Alanine aminotransferase increased

Common

Drug-induced liver injury

Not known

Skin and subcutaneous tissue disorders

Pruritus

Common

Rash

Common

Alopecia

Common

Erythema

Common

Renal and urinary disorders

Proteinuria

Common

General disorders and administration site conditions

Feeling hot

Common

Investigations

Ketones measured in urine

Very common

Albumin urine present

Common

White blood cell count decreased

Common

Description of selected adverse reactions

Flushing

In the placebo-controlled studies, the incidence of flushing (34% versus 4%) and hot flush (7% versus 2%) was increased in patients treated with Dimethyl Fumarate compared to placebo, respectively. Flushing is usually described as flushing or hot flush, but can include other events (e.g., warmth, redness, itching, and burning sensation). Flushing events tend to begin early in the course of treatment (primarily during the first month) and in patients who experience flushing, these events may continue to occur intermittently throughout treatment with Dimethyl Fumarate. In patients with flushing, the majority had flushing events that were mild or moderate in severity. Overall, 3% of patients treated with Dimethyl Fumarate discontinued due to flushing. The incidence of serious flushing, which may be characterised by generalised erythema, rash and/or pruritus, was seen in less than 1% of patients treated with Dimethyl Fumarate (see sections 4.2, 4.4 and 4.5).

Gastrointestinal

The incidence of gastrointestinal events (e.g., diarrhoea [14% versus 10%], nausea [12% versus 9%], upper abdominal pain [10% versus 6%], abdominal pain [9% versus 4%], vomiting [8% versus 5%] and dyspepsia [5% versus 3%]) was increased in patients treated with Dimethyl Fumarate compared to placebo, respectively. Gastrointestinal events tend to begin early in the course of treatment (primarily during the first month) and in patients who experience gastrointestinal events, these events may continue to occur intermittently throughout treatment with Dimethyl Fumarate. In the majority of patients who experienced gastrointestinal events, it was mild or moderate in severity. Four per cent (4%) of patients treated with Dimethyl Fumarate discontinued due to gastrointestinal events. The incidence of serious gastrointestinal events, including gastroenteritis and gastritis, was seen in 1% of patients treated with Dimethyl Fumarate (see section 4.2).

Hepatic function

Based on data from placebo-controlled studies, the majority of patients with elevations had hepatic transaminases that were <3 times the upper limit of normal (ULN). The increased incidence of elevations of hepatic transaminases in patients treated with Dimethyl Fumarate relative to placebo was primarily seen during the first 6 months of treatment. Elevations of alanine aminotransferase and aspartate aminotransferase ≥ 3 times ULN, respectively, were seen in 5% and 2% of patients treated with placebo and 6% and 2% of patients treated with Dimethyl Fumarate. Discontinuations due to elevated hepatic transaminases were <1% and similar in patients treated with Dimethyl Fumarate or placebo. Elevations in transaminases ≥ 3 times ULN with concomitant elevations in total bilirubin >2 times ULN, were not observed in placebo-controlled studies.

Increase of liver enzymes and cases of drug-induced liver injury (elevations in transaminases ≥ 3 times ULN with concomitant elevations in total bilirubin >2 times ULN), have been reported in post marketing experience following Dimethyl Fumarate administration, which resolved upon treatment discontinuation.

Lymphopenia

In the placebo-controlled studies most patients (> 98 %) had normal lymphocyte values prior to initiating treatment. Upon treatment with dimethyl fumarate, mean lymphocyte counts decreased over the first year with a subsequent plateau. On average, lymphocyte counts decreased by approximately 30 % of baseline value. Mean and median lymphocyte counts remained within normal limits. Lymphocyte counts < 0.5 x 109/l were observed in < 1 % of patients treated with placebo and 6 % of patients treated with dimethyl fumarate. A lymphocyte count < 0.2 x 109/l was observed in 1 patient treated with dimethyl fumarate and in no patients treated with placebo. In clinical studies (both controlled and uncontrolled), 41 % of patients treated with dimethyl fumarate had lymphopenia (defined in these studies as < 0.91 x 109/l). Mild lymphopenia (counts ≥ 0.8 x 109/l and < 0.91 x 109/l) was observed in 28 % of patients; moderate lymphopenia (counts ≥ 0.5 x 109/l and < 0.8 x 109/l) persisting for at least six months was observed in 10 % of patients; severe lymphopenia (counts < 0.5 x 109/l) persisting for at least six months was observed in 2 % of patients. In the group with severe lymphopenia, the majority of lymphocyte counts remained <0.5 x 109/l with continued therapy.

In addition, in an uncontrolled, prospective, post-marketing study, at week 48 of treatment with dimethyl fumarate (n=185) CD4+ T cells were moderately (counts ≥ 0.2 x 109/l to < 0.4 x 109/l) or severely (< 0.2 x 109/l) decreased in up to 37 % or 6 % of patients, respectively, while CD8+ T cells were more frequently reduced with up to 59 % of patients at counts < 0.2 x 109/l and 25 % of patients at counts < 0.1 x 109/l.

Infections, including PML and opportunistic infections

Cases of infections with John Cunningham virus (JCV) causing Progressive Multifocal Leukoencephalopathy (PML) have been reported with dimethyl fumarate (see section 4.4). PML may be fatal or result in severe disability. In one of the clinical trials, one patient taking dimethyl fumarate developed PML in the setting of prolonged severe lymphopenia (lymphocyte counts predominantly < 0.5 x 109/l for 3.5 years), with a fatal outcome. In the postmarketing setting, PML has also occurred in the presence of moderate and mild lymphopenia (> 0.5 x 109/l to < LLN, as defined by local laboratory reference range).

In several PML cases with determination of T cell subsets at the time of diagnosis of PML, CD8+ T cell counts were found to be decreased to < 0.1 x 109/l, whereas reductions in CD4+ T cells counts were variable (ranging from < 0.05 to 0.5 x 109/l) and correlated more with the overall severity of lymphopenia (< 0.5 x 109/l to < LLN). Consequently, the CD4+/CD8+ ratio was increased in these patients.

Prolonged moderate to severe lymphopenia appears to increase the risk of PML with dimethyl fumarate however, PML also occurred in patients with mild lymphopenia. Additionally, the majority of PML cases in the postmarketing setting have occurred in patients > 50 years.

Herpes zoster infections have been reported with dimethyl fumarate use. In an ongoing long-term extension study, in which 1,736 MS patients are treated with dimethyl fumarate, approximately 5 % experienced one or more events of herpes zoster, the majority of which were mild to moderate in severity. Most subjects, including those who experienced a serious herpes zoster infection, had lymphocyte counts above the lower limit of normal. In a majority of subjects with concurrent lymphocyte counts below the LLN, lymphopenia was rated moderate or severe.

In the post-marketing setting, most cases of herpes zoster infection were nonserious and resolved with treatment. Limited data is available on ALC in patients with herpes zoster infection in the post-marketing setting. However, when reported, most patients experienced moderate (< 0.8 x 109/l to 0.5 x 109/l) or severe (< 0.5 x 109/l to 0.2 x 109/l) lymphopenia (see section 4.4).

Laboratory abnormalities

In the placebo-controlled studies, measurement of urinary ketones (1+ or greater) was higher in patients treated with dimethyl fumarate (45 %) compared to placebo (10 %). No untoward clinical consequences were observed in clinical trials.

Levels of 1,25-dihydroxyvitamin D decreased in dimethyl fumarate treated patients relative to placebo (median percentage decrease from baseline at 2 years of 25 % versus 15 %, respectively) and levels of parathyroid hormone (PTH) increased in dimethyl fumarate treated patients relative to placebo (median percentage increase from baseline at 2 years of 29 % versus 15 %, respectively). Mean values for both parameters remained within normal range.

A transient increase in mean eosinophil counts was seen during the first 2 months of therapy.

Paediatric population

In a 96 week open label, randomised active controlled trial in paediatric patients with RRMS aged 10 to less than 18 years (120 mg twice a day for 7 days followed by 240 mg twice a day for the remainder of treatment; study population, n=78), the safety profile in paediatric patients appeared similar to that previously observed in adult patients.

The paediatric clinical trial design differed from the adult placebo-controlled clinical trials. Therefore, a contribution of clinical trial design to numerical differences in adverse reactions between the paediatric and adult populations, cannot be excluded.

The following adverse events were more frequently reported (≥ 10%) in the paediatric population than in the adult population:

• Headache was reported in 28% of patients treated with Dimethyl Fumarate versus 36% in patients treated with interferon beta-1a.

• Gastrointestinal disorders were reported in 74% of patients treated with Dimethyl Fumarate versus 31% in patients treated with interferon beta-1a. Among them, abdominal pain and vomiting were the most frequently reported with Dimethyl Fumarate.

• Respiratory, thoracic and mediastinal disorders were reported in 32% of patients treated with Dimethyl Fumarate versus 11% in patients treated with interferon beta-1a. Among them, oropharyngeal pain and cough were the most frequently reported with Dimethyl Fumarate.

• Dysmenorrhea was reported in 17% of patients treated with Dimethyl Fumarate versus 7% of patients treated with interferon beta-1a.

In a small 24 week open-label uncontrolled study in paediatric patients with RRMS aged 13 to 17 years (120 mg twice a day for 7 days followed by 240 mg twice a day for the remainder of treatment; safety population, n=22), followed by a 96 week extension study (240 mg twice per day; safety population n=20), the safety profile appeared similar to that observed in adult patients.

There are limited data available in children between 10 and 12 years old. The safety and efficacy of Dimethyl Fumarate in children aged less than 10 years have not yet been established.

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

Cases of overdose with Dimethyl Fumarate have been reported. The symptoms described in these cases were consistent with the known adverse reaction profile of Dimethyl Fumarate.

There are no known therapeutic interventions to enhance elimination of Dimethyl Fumarate nor is there a known antidote. In the event of overdose, it is recommended that symptomatic supportive treatment be initiated as clinically indicated.

5. Pharmacological properties

5.1 Pharmacodynamic properties

Pharmacotherapeutic group: Antineoplastic and immunomodulating agents, ATC Code: L04AX07

Mechanism of Action

The mechanism by which dimethyl fumarate exerts therapeutic effects in multiple sclerosis is not fully understood. Preclinical studies indicate that dimethyl fumarate pharmacodynamic responses appear to be primarily mediated through activation of the nuclear factor (erythroid-derived 2)-like 2 (Nrf2) transcriptional pathways. Dimethyl fumarate has been shown to up regulate Nrf2-dependent antioxidant genes in patients (e.g. NAD(P)H dehydrogenase, quinone 1; [NQO1]).

Pharmacodynamic Effects

Effects on the immune system

In preclinical and clinical studies, dimethyl fumarate demonstrated antiinflammatory and immunomodulatory properties. Dimethyl fumarate and monomethyl fumarate, the primary metabolite of dimethyl fumarate, significantly reduced immune cell activation and subsequent release of proinflammatory cytokines in response to inflammatory stimuli in preclinical models.

In clinical studies with psoriasis patients, dimethyl fumarate affected lymphocyte phenotypes through a down-regulation of pro-inflammatory cytokine profiles (TH1, TH17), and biased towards anti-inflammatory production (TH2). Dimethyl fumarate demonstrated therapeutic activity in multiple models of inflammatory and neuroinflammatory injury. In Phase 3 studies in MS patients, upon treatment with dimethyl fumarate mean lymphocyte counts decreased on average by approximately 30 % of their baseline value over the first year with a subsequent plateau.

Clinical efficacy and safety

Two, 2-year, randomised, double-blind, placebo-controlled studies [Study 1 (DEFINE) with 1,234 subjects and Study 2 (CONFIRM) with 1,417 subjects] of subjects with relapsing remitting multiple sclerosis (RRMS) were performed. Subjects with progressive forms of MS were not included in these studies.

Efficacy (see Table 2) and safety were demonstrated in subjects with Expanded Disability Status Scale (EDSS) scores ranging from 0 to 5 inclusive, who had experienced at least 1 relapse during the year prior to randomisation, or, in the 6 weeks before randomisation had a brain Magnetic Resonance Imaging (MRI) demonstrating at least one gadolinium-enhancing (Gd+) lesion.

Study 2 contained a rather-blinded (i.e., study physician/ investigator assessing the response to study treatment was blinded) reference comparator of glatiramer acetate.

In Study 1, patients had the following median baseline characteristics: age 39 years, disease duration 7.0 years, EDSS score 2.0. In addition, 16 % of patients had an EDSS score >3.5, 28% had ≥ 2 relapses in the prior year and 42 % had previously received other approved MS treatments. In the MRI cohort 36 % of patients entering the study had Gd+ lesions at baseline (mean number of Gd+ lesions 1.4).

In Study 2, patients had the following median baseline characteristics: age 37 years, disease duration 6.0 years, EDSS score 2.5. In addition, 17 % of patients had an EDSS score > 3.5, 32 % had ≥ 2 relapses in the prior year and 30 % had previously received other approved MS treatments. In the MRI cohort 45 % of patients entering the study had Gd+ lesions at baseline (mean number of Gd+ lesions 2.4).

Compared to placebo, subjects treated with Dimethyl fumarate had a clinically meaningful and statistically significant reduction on: the primary endpoint in Study 1, proportion of subjects relapsed at 2 years; and the primary endpoint in Study 2, annualised relapse rate at 2 years.

The annualised relapse rate for glatiramer acetate and placebo was 0.286 and 0.401 respectively in Study 2, corresponding to a reduction of 29 % (p=0.013), which is consistent with approved prescribing information.

Table 2: Efficacy and safety in controlled studies

DEFINE

CONFIRM

Placebo

Dimethyl fumarate

240 mg twice a day

Placebo

Dimethyl fumarate

240 mg twice a day

Glatiramer acetate

Clinical Endpoints a

No. subjects

408

410

363

359

350

Annualised relapse rate

0.364

0.172 ***

0.401

0.224 ***

0.286 *

Rate ratio

(95 % CI)

0.47

(0.37, 0.61)

0.56

(0.42, 0.74)

0.71

(0.55, 0.93)

Proportion relapsed

0.461

0.270 ***

0.410

0.291 **

0.321 **

Hazard ratio

(95 % CI)

0.51

(0.40, 0.66)

0.66

(0.51, 0.86)

0.71

(0.55, 0.92)

Proportion with 12-week confirmed disability progression

0.271

0.164 **

0.169

0.128 #

0.156 #

Hazard ratio

(95 % CI)

0.62

(0.44, 0.87)

0.79

(0.52, 1.19)

0.93

(0.63, 1.37)

Proportion with 24-week confirmed disability progression

0.169

0.128 #

0.125

0.078 #

0.108 #

Hazard ratio

(95 % CI)

0.77

(0.52, 1.14)

0.62

(0.37, 1.03)

0.87

(0.55, 1.38)

MRI Endpoints b

No. subjects

165

152

144

147

161

Mean (median) number of new or newly enlarging T2 lesions over 2 years

16.5

(7.0)

3.2

(1.0) ***

19.9

(11.0)

5.7

(2.0) ***

9.6

(3.0) ***

Lesion mean ratio (95% CI)

0.15

(0.10, 0.23)

0.29

(0.21, 0.41)

0.46

(0.33, 0.63)

Mean (median) number of Gd lesions at 2 years

1.8

(0)

0.1

(0) ***

2.0

(0.0)

0.5

(0.0) ***

0.7

(0.0) **

Odds ratio

(95 % CI)

0.10

(0.05, 0.22)

0.26

(0.15, 0.46)

0.39

(0.24, 0.65)

Mean (median) number of new T1 hypointense lesions over 2 years

5.7

(2.0)

2.0

(1.0) ***

8.1

(4.0)

3.8

(1.0) ***

4.5

(2.0) **

Lesion mean ratio (95 % CI)

0.28

(0.20, 0.39)

0.43

(0.30, 0.61)

0.59

(0.42, 0.82)

a All analyses of clinical endpoints were intent-to-treat;

b MRI analysis used MRI cohort

* P-value <0.05;

** P-value <0.01;

*** P-value <0.0001;

#not statistically significant

Efficacy in patients with high disease activity

Consistent treatment effect on relapses in a subgroup of patients with high disease activity was observed, whilst the effect on time to 3-month sustained disability progression was not clearly established. Due to the design of the studies, high disease activity was defined as follows:

- patients with 2 or more relapses in one year, and with one or more Gd-enhancing lesions on brain MRI (n=42 in DEFINE; n=51 in CONFIRM) or,

- patients who have failed to respond to a full and adequate course (at least one year of treatment) of beta-interferon, having had at least 1 relapse in the previous year while on therapy, and at least 9 T2-hyperintense lesions in cranial MRI or at least 1 Gdenhancing lesion, or patients having an unchanged or increased relapse rate in the prior year as compared to the previous 2 years (n=177 in DEFINE; n=141 in CONFIRM).

Paediatric population

Dimethyl fumarate was evaluated in a prospective open-label, uncontrolled study in 22 paediatric patients with RRMS aged 13 to 17 years (4 patients aged ≤ 14 years). Subjects received dimethyl fumarate 120 mg twice a day for 7 days followed by 240 mg twice a day for 24 weeks. The median number of new or newly enlarging T2 hyperintense lesions changed from 2 in the 8-week pre-treatment evaluation period to 0 in the final 8 weeks of the treatment period (median change -2, n=16).

Patients subsequently entered an extension study for a further 96 weeks. Among the 10 patients with MRI data between weeks 64 and week 72 of the extension study, the median number of subjects with new or newly enlarging T2 hyperintense lesions was 0 (range 0,2). Over the full treatment period (120week), ARR was 0.2 representing an 84.5 % relative reduction in relapses (n=20; 95 % CI [66.8, 92.8], p < 0.0001), when compared to the year prior to treatment initiation. These data should be considered cautiously regarding limitations of the study design (no control arm, pre-versus post-dose comparison) (see section 4.2).

5.2 Pharmacokinetic properties

Orally administered dimethyl fumarate undergoes rapid pre-systemic hydrolysis by esterases and is converted to its primary metabolite, monomethyl fumarate, which is also active. Dimethyl fumarate is not quantifiable in plasma following oral administration of dimethyl fumarate. Therefore, all pharmacokinetic analyses related to dimethyl fumarate were performed with plasma monomethyl fumarate concentrations. Pharmacokinetic data were obtained in subjects with multiple sclerosis and healthy volunteers.

Absorption

The Tmax of monomethyl fumarate is 2 to 2.5 hours. As dimethyl fumarate gastro-resistant hard capsules contain minitablets, which are protected by an enteric coating, absorption does not commence until they leave the stomach (generally less than 1 hour). Following 240 mg twice a day administered with food, the median peak (Cmax) was 1.72 mg/l and overall area under the curve (AUC) exposure was 8.02 h.mg/l in subjects with multiple sclerosis. Overall, Cmax and AUC increased approximately dose-proportionally in the dose range studied (120 mg to 360 mg). In subjects with multiple sclerosis, two 240 mg doses were administered 4 hours apart as part of three times a day dosing regimen. This resulted in a minimal accumulation of exposure yielding an increase in the median Cmax of 12 % compared to the twice daily dosing (1.72 mg/l for twice daily compared to 1.93 mg/l for three times daily) with no safety implications.

Food does not have a clinically significant effect on exposure of dimethyl fumarate. However, dimethyl fumarate should be taken with food due to improved tolerability with respect to flushing or gastrointestinal adverse events (see section 4.2).

Distribution

The apparent volume of distribution following oral administration of 240 mg dimethyl fumarate varies between 60 l and 90 l. Human plasma protein binding of monomethyl fumarate generally ranges between 27 % and 40 %.

Biotransformation

In humans, dimethyl fumarate is extensively metabolised with less than 0.1 % of the dose excreted as unchanged dimethyl fumarate in urine. It is initially metabolised by esterases, which are ubiquitous in the gastrointestinal tract, blood and tissues, before it reaches the systemic circulation. Further metabolism occurs through the tricarboxylic acid cycle, with no involvement of the cytochrome P450 (CYP) system.

A single 240 mg 14C-dimethyl fumarate dose study identified glucose as the predominant metabolite in human plasma. Other circulating metabolites included fumaric acid, citric acid and monomethyl fumarate. The downstream metabolism of fumaric acid occurs through the tricarboxylic acid cycle, with exhalation of CO2 serving as a primary route of elimination.

Elimination

Exhalation of CO2 is the primary route of dimethyl fumarate elimination accounting for 60 % of the dose. Renal and faecal elimination are secondary routes of elimination, accounting for 15.5 % and 0.9 % of the dose respectively.

The terminal half-life of monomethyl fumarate is short (approximately 1 hour) and no circulating monomethyl fumarate is present at 24 hours in the majority of individuals. Accumulation of parent drug or monomethyl fumarate does not occur with multiple doses of dimethyl fumarate at the therapeutic regimen.

Linearity

Dimethyl fumarate exposure increases in an approximately dose proportional manner with single and multiple doses in the 120 mg to 360 mg dose range studied.

Pharmacokinetics in special patient groups

Based on the results of Analysis of Variance (ANOVA), body weight is the main covariate of exposure (by Cmax and AUC) in RRMS subjects, but did not affect safety and efficacy measures evaluated in the clinical studies. Gender and age did not have a clinically significant impact on the pharmacokinetics of dimethyl fumarate. The pharmacokinetics in patients aged 65 and over has not been studied.

Paediatric population

The pharmacokinetic profile of 240 mg dimethyl fumarate twice a day was evaluated in a small, open-label, uncontrolled study in patients with RRMS aged 13 to 17 years (n=21). The pharmacokinetics of dimethyl fumarate in these adolescent patients was consistent with that previously observed in adult patients (Cmax: 2.00± 1.29 mg/l; AUC0-12hr: 3.62± 1.16 h.mg/l, which corresponds to an overall daily AUC of 7.24 h.mg/l).

Renal impairment

Since the renal pathway is a secondary route of elimination for dimethyl fumarate accounting for less than 16 % of the dose administered, evaluation of pharmacokinetics in individuals with renal impairment was not conducted.

Hepatic impairment

As dimethyl fumarate and monomethyl fumarate are metabolised by esterases, without the involvement of the CYP450 system, evaluation of pharmacokinetics in individuals with hepatic impairment was not conducted.

5.3 Preclinical safety data

The adverse reactions described in the Toxicology and Reproduction toxicity sections below were not observed in clinical studies, but were seen in animals at exposure levels similar to clinical exposure levels.

Mutagenesis

Dimethyl fumarate and monomethyl fumarate were negative in a battery of in vitro assays (Ames, chromosomal aberration in mammalian cells). Dimethyl fumarate was negative in the in vivo micronucleus assay in the rat.

Carcinogenesis

Carcinogenicity studies of dimethyl fumarate were conducted for up to 2 years in mice and rats. Dimethyl fumarate was administered orally at doses of 25, 75, 200 and 400 mg/kg/day in mice, and at doses of 25, 50, 100, and 150 mg/kg/day in rats. In mice, the incidence of renal tubular carcinoma was increased at 75 mg/kg/day, at equivalent exposure (AUC) to the recommended human dose. In rats, the incidence of renal tubular carcinoma and testicular Leydig cell adenoma was increased at 100 mg/kg/day, approximately 2 times higher exposure than the recommended human dose. The relevance of these findings to human risk is unknown.

The incidence of squamous cell papilloma and carcinoma in the non-glandular stomach (forestomach) was increased at equivalent exposure to the recommended human dose in mice and below exposure to the recommended human dose in rats (based on AUC). The forestomach in rodents does not have a human counterpart.

Toxicology

Nonclinical studies in rodent, rabbits, and monkeys were conducted with a dimethyl fumarate suspension (dimethyl fumarate in 0.8 % hydroxypropyl methylcellulose) administered by oral gavage. The chronic dog study was conducted with oral administration of the dimethyl fumarate capsule. Kidney changes were observed after repeated oral administration of dimethyl fumarate in mice, rats, dogs, and monkeys. Renal tubule epithelial regeneration, suggestive of injury, was observed in all species. Renal tubular hyperplasia was observed in rats with lifetime dosing (2-year study). In dogs that received daily oral doses of dimethyl fumarate for 11 months, the margin calculated for cortical atrophy was observed at 3 times the recommended dose based on AUC. In monkeys that received daily oral doses of dimethyl fumarate for 12 months, single cell necrosis was observed at 2 times the recommended dose based on AUC. Interstitial fibrosis and cortical atrophy were observed at 6 times the recommended dose based on AUC. The relevance of these findings to humans is not known.

In the testes, degeneration of the seminiferous epithelium was seen in rats and dogs. The findings were observed at approximately the recommended dose in rats and 3 times the recommended dose in dogs (AUC basis). The relevance of these findings to humans is not known.

Findings in the forestomach of mice and rats consisted of squamous epithelial hyperplasia and hyperkeratosis; inflammation; and squamous cell papilloma and carcinoma in studies of 3 months or longer in duration. The forestomach of mice and rats does not have a human counterpart.

Reproduction toxicity

Oral administration of dimethyl fumarate to male rats at 75, 250, and 375 mg/kg/day prior to and during mating had no effects on male fertility up to the highest dose tested (at least 2 times the recommended dose on an AUC basis). Oral administration of dimethyl fumarate to female rats at 25, 100, and 250 mg/kg/day prior to and during mating, and continuing to Day 7 of gestation, induced reduction in the number of oestrous stages per 14 days and increased the number of animals with prolonged dioestrus at the highest dose tested (11 times the recommended dose on an AUC basis). However, these changes did not affect fertility or the number of viable foetuses produced.

Dimethyl fumarate has been shown to cross the placental membrane into fetal blood in rats and rabbits, with ratios of foetal to maternal plasma concentrations of 0.48 to 0.64 and 0.1 respectively. No malformations were observed at any dose of dimethyl fumarate in rats or rabbits. Administration of dimethyl fumarate at oral doses of 25, 100, and 250 mg/kg/day to pregnant rats during the period of organogenesis resulted in maternal adverse effects at 4 times the recommended dose on an AUC basis, and low fetal weight and delayed ossification (metatarsals and hindlimb phalanges) at 11 times the recommended dose on an AUC basis. The lower fetal weight and delayed ossification were considered secondary to maternal toxicity (reduced body weight and food consumption).

Oral administration of dimethyl fumarate at 25, 75, and 150 mg/kg/day to pregnant rabbits during organogenesis had no effect on embryo-foetal development and resulted in reduced maternal body weight at 7 times the recommended dose and increased abortion at 16 times the recommended dose, on an AUC basis.

Oral administration of dimethyl fumarate at 25, 100, and 250 mg/kg/day to rats during pregnancy and lactation resulted in lower body weights in the F1 offspring, and delays in sexual maturation in F1 males at 11 times the recommended dose on an AUC basis. There were no effects on fertility in the F1 offspring. The lower offspring body weight was considered secondary to maternal toxicity.

Two toxicity studies in juvenile rats with daily oral administration of dimethyl fumarate from postnatal day (PND) 28 through PND 90 to 93 (equivalent to approximately 3 years and older in humans) revealed similar target organ toxicities in the kidney and forestomach as observed in adult animals. In the first study, dimethyl fumarate did not affect development, neurobehavior or male and female fertility up to the highest dose of 140 mg/kg/day (approximately 4.6 times the recommended human dose based on limited AUC data in paediatric patients). Likewise, no effects on male reproductive and accessory organs were observed up to the highest dimethyl fumarate dose of 375 mg/kg/day in the second study in male juvenile rats (about 15-times the putative AUC at the recommended paediatric dose). However, decreased bone mineral content and density in the femur and lumbar vertebrae were evident in male juvenile rats. Bone densitometry changes were also observed in juvenile rats following oral diroximel fumarate administration, another fumaric ester that is metabolised to the same active metabolite monomethyl fumarate in vivo. The NOAEL for the densitometry changes in juvenile rats is approximately 1.5 times the presumptive AUC at the recommended paediatric dose. A relation of the bone effects to lower body weight is possible, but the involvement of a direct effect cannot be excluded. The bone findings are of limited relevance for adult patients. The relevance for paediatric patients is not known.

6. Pharmaceutical particulars

6.1 List of excipients

Capsule contents (enteric-coated minitablets)

Microcrystalline cellulose

Crospovidone

Talc

Povidone K-30

Silica, colloidal anhydrous

Magnesium stearate

Triethyl citrate

Methacrylic acid/ethyl acrylate copolymer (1:1)

Hydroxypropyl methyl cellulose

Titanium dioxide (E 171)

Triacetin

Capsule shell

Gelatin

Titanium dioxide (E 171)

Brilliant blue FCF-FD&C Blue 1 (E 133)

Yellow iron oxide (E 172)

Capsule print (black ink)

Shellac

Potassium hydroxide

Propylene glycol

Black iron oxide (E 172)

Strong ammonia solution

Purified water

6.2 Incompatibilities

Not applicable.

6.3 Shelf life

3 years

6.4 Special precautions for storage

This medicinal product does not require any special temperature storage conditions.

6.5 Nature and contents of container

HDPE bottles with PP/HDPE caps with seal and silica gel desiccant cannister containing 100 capsules.

Carton box containing Al/Al blisters of 7 capsules each and a heat-sealed blister card.

Pack size of 14 capsules (blisters) or 100 capsules (bottle).

Not all pack sizes may be marketed.

6.6 Special precautions for disposal and other handling

No special requirements.

7. Marketing authorisation holder

Genus Pharmaceuticals Ltd. (trading as 'STADA')

Linthwaite

Huddersfield

HD7 5QH

UK

8. Marketing authorisation number(s)

PLGB 06831/0448

9. Date of first authorisation/renewal of the authorisation

03/11/2023

10. Date of revision of the text

03/11/2023

Genus Pharmaceuticals
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