Xoflusa, 40 mg 2 pcs

Indications

Treatment of influenza in patients 12 years of age and older who have influenza symptoms for 48 hours or less and who have no additional medical conditions.

The treatment of influenza in patients 12 years of age and older who have influenza symptoms for up to 48 hours and who are at high risk for influenza complications.

Limitations of Use

Influenza viruses change over time, and factors such as virus type or subtype, emergence of resistance, or changes in viral virulence may reduce the clinical benefit of antiviral drugs. When deciding whether to use Xoflusa®, the available information about the susceptibility of circulating strains of influenza virus to the drug should be reviewed.

Active ingredient

Composition

One film-coated tablet, 40 mg contains:

active ingredient: baloxavir marboxil – 40 mg;

excipients: lactose monohydrate – 155.8 mg, croscarmellose sodium – 11 mg, povidone K25 – 11 mg, microcrystalline cellulose – 22.8 mg, sodium stearyl fumarate – 3.4 mg;

coating: Opadry White 03A48081 (hypromellose, talc, titanium dioxide (E171)) – 7.6 mg, talc – 0.3 mg.

How to take, the dosage

General Guidelines

Therapy with Xoflusa® should be started within 48 hours after the onset of flu symptoms.

Adults and children over 12 years of age

The drug Xoflusa® is used once, either with food or on an empty stomach (see Pharmacological properties).

The recommended daily dose of Xofluzam® as a function of body weight is shown in Table 2.

Table 2. Dose of Xoflusa® as a function of a patient’s body weight.

Patient body weight(kg) Recommended dose to take
40 kg to <80 kg 40 mg
≥80 kg 80 mg

Dosage in special cases

Patients in children

The safety and effectiveness of Xofluz® in children and adolescents ˂12 years of age have not been established. For recommendations on the use of Xoflusa® in adolescents ≥12 years of age, see the “General Recommendations” subsection above.

Elderly patients

Dose adjustment in elderly patients ≥65 years of age is not necessary (see Pharmacological properties, subsection “Pharmacokinetics in special patient groups”, section “Elderly patients”).

Patients with impaired renal function

Population pharmacokinetics analysis showed no clinically significant effect of renal function on baloxavir pharmacokinetics in patients with a creatinine clearance (CrCl) ≥50 mL/min. The effect of severe renal function impairment on the pharmacokinetics of baloxavir marboxil or its active metabolite baloxavir has not been studied.

Patients with hepatic impairment

Dose adjustment in patients with mild (Child-Pugh class A) or moderate (Child-Pugh class B) hepatic impairment is not required (see “Pharmacological properties of baloxivir. See “Pharmacological properties”, subsection “Pharmacokinetics in special patient groups”, section “Patients with impaired hepatic function”). The use of Xoflusa® in patients with severe hepatic impairment has not been studied.

Interaction

No clinically significant drug interactions are expected between baloxavir marboxil or its active metabolite baloxavir and substrates, cytochrome P450 inhibitors or inducers (CYP isoenzymes), uridine-5-diphosphate glucuronyltransferase (UGT) enzyme inhibitors, and carriers in the gut, kidney or liver.

Polyvalent cation-containing drugs can decrease the plasma concentration of baloxavir. Xoflusa® should not be taken with laxatives or antacids containing polyvalent cations or supplements containing iron, zinc, selenium, calcium, magnesium.

Interaction with vaccines

The interaction of the drug Xoflusa

sup>® with intranasal live attenuated influenza vaccine (LAIV) has not been studied. Concomitant use of antiviral drugs may inhibit viral replication of LAIV and thus reduce the effectiveness of LAIV vaccination. The interaction of Xoflusa® with inactivated influenza vaccine has not been studied.

Influence of other drugs on baloxavir marboxil or its active metabolite baloxavir

Itraconazole, a P-glycoprotein inhibitor (P-gp), increased the Cmax and AUC0-∞ of baloxavir by 1.33-fold and 1.23-fold, respectively. The increase in these values was not considered clinically significant.

The UST enzyme inhibitor probenecid reduced the Cmax and AUC0-∞ of baloxavir by 21% and 25%, respectively. The decrease in these values was not considered clinically significant.

The effect of baloxavir marboxil or its active metabolite baloxavir on other drugs

In in vitro

Special Instructions

Hypersensitivity reactions

In the post-registration use of Xoflusa

sup>® cases of anaphylaxis, urticaria, angioedema and erythema multiforme have been reported. In case of allergic-like reactions or suspected allergic reactions, appropriate treatment should be started. The use of Xoflusa® is contraindicated in patients with a history of hypersensitivity to Xoflusa® (see sections “Contraindications” and “Side effects”).

Risk of bacterial infections

The evidence of efficacy of Xofluzsup>® for any disease caused by any pathogen other than influenza viruses is not available. Serious bacterial infections may start with flu-like symptoms, may accompany influenza, or may occur as a complication of influenza. Xoflusa® does not prevent such complications. When prescribing Xoflusa®, the potential occurrence of secondary bacterial infections should be considered and appropriate treatment prescribed.

Instructions for disposal of unused or expired medication

The release of the medication into the environment should be minimized. The drug should not be disposed of in wastewater or with household waste.

Disposal of unused medication or consumables should be done according to local requirements.

Influence on driving and operating ability

There have been no studies of the effect of Xoflusa® on driving and operating ability.

Synopsis

Contraindications

He has a history of hypersensitivity to baloxavir marboxil or other excipients of the drug (see section “Adverse effects”, subsection “Post-registration use”).

Simultaneous use with laxatives or antacids containing polyvalent cations, as well as supplements containing iron, zinc, selenium, calcium, magnesium (decrease in plasma concentration of baloxavir).

Lactose intolerance, lactase deficiency, glucose-galactose malabsorption.

Children under 12 years of age.

With caution

Kidney function impairment.

Serious impairment of liver function.

Side effects

Because clinical studies have been conducted under different conditions, the frequency of adverse drug reactions observed in clinical studies of a drug cannot be directly compared to the frequency of adverse reactions observed in clinical studies of another drug. The frequency of adverse drug reactions observed in clinical studies may not reflect the frequency of adverse reactions in actual practice.

The safety profile of Xofluz® is based on data from 3 placebo-controlled clinical trials in which 1640 patients received the drug: 1334 patients (81%) aged 18 to 64 years, 209 patients (13%) aged ≥65 years, and 97 patients (6%) aged 12 to 17 years. These studies included adult patients and adolescents without additional medical conditions (N=910) as well as patients at high risk for influenza complications (N=730). Of all patients, 1,440 received Xoflusa® at the recommended dose.

Post-registration use

. The following adverse drug reactions were identified during post-registration use of Xofluz®. Because these adverse reactions were reported voluntarily in a patient population of unknown size, it is not possible to reliably estimate the frequency of their development or whether they are associated with Xoflusa®.

Psychiatric disorders: delirium, abnormal behavior, and hallucinations.

Gastrointestinal tract disorders: vomiting, bloody diarrhea, melena, colitis.

Skin and subcutaneous tissue disorders: rash, urticaria, erythema multiforme.

General disorders and disorders at the site of administration:Facial, eyelid or tongue edema, dysphonia, angioedema, anaphylactic reactions, anaphylactic shock, anaphylactoid reactions.

Overdose

No cases of overdose have been reported.

Therapy: There is no known specific antidote for Xoflusa®. In case of overdose, standard supportive medical care should be given based on the patient’s signs and symptoms of overdose. It is unlikely that baloxavir can be eliminated in significant amounts by dialysis due to its high binding to serum proteins.

Pregnancy use

Fertility

Baloxavir marboxil has no effect on fertility according to studies in animals.

Pregnancy

There have been no separate controlled studies of Xoflusa® in pregnant women. The potential risk of Xoflusa® in pregnant women is unknown. Xoflusa® should not be administered during pregnancy unless the potential benefit exceeds the possible risk to the fetus.

Doclinical data

Baloxavir marboxil has not caused malformations in rats or rabbits. High-dose levels of baloxavir marboxil used in pregnant rabbits had maternal toxicity, leading to the development of miscarriage and an increased incidence of minor skeletal abnormalities in rabbits, but there were no malformations. These effects were not noted in rats.

partum and delivery

The safety of Xofluz® during labor has not been established.

Breastfeeding period

It is currently unknown whether baloxavir marboxil and its active metabolite baloxavir can penetrate human breast milk. When administered at a dose of 1 mg/kg in lactating rats, baloxavir marboxil or its metabolites were secreted into milk.

Hence, the decision to discontinue breastfeeding or to initiate treatment with Xoflusa® should be based on the potential benefit of the drug to the nursing mother as well as the potential risk to the baby.