Mitexan

Overdose

Reports of inadvertent overdose and observations from a high-dose tolerability study in healthy volunteers showed that, in adults, single doses in the range of approximately 4g to 7g of Mitexan can cause symptoms such as nausea, vomiting, abdominal pain/colic, diarrhoea, headache, fatigue, limb and joint pains, rash, flushing, hypotension, bradycardia, tachycardia, paresthesia, fever, and bronchospasm.

A markedly increased rate of nausea, vomiting and diarrhoea has also been found in oxazaphosphorine-treated patients receiving > 80 mg Mitexan per kg per day intravenously compared with patients receiving lower doses or hydration treatment only.

A specific antidote to Mitexan is not known.

Contraindications

Known hypersensitivity to Mitexan or any of the excipients.

Incompatibilities

Mitexan is incompatible with platinum derivatives (e.g. Cisplatin, carboplatin and nitrogen mustard) and must not be mixed in the same infusion solution.

Mixing Mitexan and epirubicin leads to inactivation of epirubicin and should be avoided.

Undesirable effects

The most frequently occurring adverse reactions (> 10%) associated with use of Mitexan are: headache, infusion site reactions, abdominal pain/colic, lightheadedness, lethargy/drowsiness, pyrexia, rash, diarrhoea, nausea, flushing, and influenza-like illness.

The most severe adverse reactions associated with use of Mitexan are: bullous skin reactions, anaphylaxis, and drug rash with eosinophilia and systemic symptoms (DRESS).

Because Mitexan is used in combination with oxazaphosphorines or oxazaphosphorine- containing combination chemotherapy, it is often difficult to distinguish adverse reactions that may be due to Mitexan from those caused by concomitantly administered cytotoxic agents.

ADR frequency is based upon the following scale: Very common (>1/10); Common (>1/100 - <1/10), Uncommon (>1/1,000 - <1/100), Rare (>1/10,000 - <1/1,000), Very rare (<1/10,000), Unknown (adverse reactions reported in the post-marketing experience)

System Organ Class (SOC)

Adverse Reaction

Frequency

BLOOD AND LYMPHATIC SYSTEM DISORDERS

Lymphadenopathy

Common

IMMUNE SYSTEM DISORDERS

Anaphylaxis

Hypersensitivity

Unknown

Unknown

METABOLISM AND NUTRITION DISORDERS

Decreased appetite

Feeling of dehydration

Common

Common

PSYCHIATRIC DISORDERS

Insomnia

Nightmare

Common

Common

NERVOUS SYSTEM DISORDERS

Headache

Light-headedness

Lethargy/Drowsiness

Dizziness

Paresthesia

Hyperesthesia

Syncope

Hypoesthesia

Disturbance in attention

Very common

Very common

Very common

Common

Common

Common

Common

Common

Common

EYE DISORDERS

Conjunctivitis

Photophobia

Vision blurred

Common

Common

Common

CARDIAC DISORDERS

Palpitations

Tachycardia

Common

Unknown

VASCULAR DISORDERS

Flushing

Hypotension

Very common

Unknown

RESPIRATORY, THORACIC, AND MEDIASTINAL DISORDERS

Nasal congestion

Cough

Pleuritic pain

Dry mouth

Bronchospasm

Dyspnea

Laryngeal discomfort

Epistaxis

Respiratory distress

Hypoxia

Common

Common

Common

Common

Common

Common

Common

Common

Unknown

Unknown

GASTROINTESTINAL DISORDERS

Abdominal pain/colic

Nausea

Diarrhoea

Mucosal irritation1

Flatulence

Vomiting

Burning pain (substernal / epigastric)

Constipation

Gingival bleeding

Very common

Very common

Very common

Common

Common

Common

Common

Common

Common

HEPATOBILIARY DISORDERS

Transaminases increased

Common

SKIN AND SUBCUTANEOUS TISSUE DISORDERS

Rash2

Pruritus

Hyperhidrosis

Erythema multiforme

Drug rash 3

Ulcerations and/or bullae/blistering 4

Angioedema

Urticaria

Burning sensation

Erythema

Very common

Common

Common

Unknown

Unknown

Unknown

Unknown

Unknown

Unknown

Unknown

MUSCULOSKELETAL AND CONNECTIVE TISSUE DISORDERS

Arthralgia

Back pain

Myalgia

Pain in extremity

Pain in jaw

Common

Common

Common

Common

Common

RENAL AND URINARY DISORDERS

Dysuria

Acute renal failure

Common

Unknown

GENERAL DISORDERS AND ADMINISTRATIVE SITE CONDITIONS

Infusion site reactions

- Infusion site pruritus

- Infusion site rash

- Infusion site pain

- Infusion site erythema

- Infusion site urticaria

- Infusion site swelling

Pyrexia

Influenza-like illness

Rigors

Fatigue

Chest pain

Malaise

Face oedema

Oedema peripheral

Asthenia

Very common

Very common

Very common

Common

Common

Common

Common

Very common

Very common

Common

Common

Common

Common

Unknown

Unknown

Unknown

INVESTIGATIONS

Activated partial thromboplastin time prolonged

Unknown

1Oral, rectal

2Including nonpruritic, pruritic, erythema/erythematous, eczematous, papular, and/or macular rashes.

3with eosinophilia and systemic symptoms

4mucocutaneous, mucosal, oral, vulvovaginal, anorectal

- Time to onset and experience with re-exposure

In these studies, some subjects experienced their events on first exposure to Mitexan and others after the second or third exposure. In general, the complete spectrum of symptoms experienced by a subject developed over a period of several hours.

Some subjects experienced no further reactions after their initial event while others experienced an exacerbation of events upon repeated dosing.

- Infusion site reactions

In some subjects experiencing local cutaneous infusion site reactions, subsequent exposure to Mitexan resulted in a cutaneous event in other areas.

- Cutaneous/mucosal reactions

Cutaneous and mucosal reactions were reported to occur after both intravenous and oral Mitexan. These reactions included rashes, pruritus, flushing, mucosal irritation, pleuritic pain, and conjunctivitis. Approximately one-quarter of subjects with any event experienced cutaneous/mucosal reactions in conjunction with other adverse symptoms, which included, dyspnea, fever, headache, gastrointestinal symptoms, drowsiness, malaise, myalgia, and influenza-like symptoms.

- Gastrointestinal reactions

Gastrointestinal reactions reported in healthy subjects included nausea, vomiting, diarrhea, abdominal pain/colic, epigastric pain/burning, constipation, and flatulence and were reported to occur after intravenous and oral Mitexan administration.

- In-vivo effect on lymphocyte counts

In pharmacokinetics studies in healthy volunteers, administration of single doses of Mitexan was commonly associated with a rapid (within 24 hours) and in some cases marked decrease in lymphocyte count, which was generally reversible within 1 week of administration. Data from studies with repeated dosing over several days are insufficient to characterize the time course of lymphocyte count changes under such conditions.

- In-vivo effect on serum phosphorus levels

In pharmacokinetics studies in healthy volunteers, administration of Mitexan on single or multiple days was in some cases associated with moderate transient increases in serum phosphorus concentration.

These phenomena should be considered when interpreting laboratory results.

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.

Website: www.mhra.gov.uk/yellowcard

Preclinical safety data

Nothing relevant.

Therapeutic indications

For the prevention of urothelial toxicity including haemorrhagic cystitis, microhaematuria and macrohaematuria in patients treated with ifosfamide and cyclophosphamide, in doses considered to be urotoxic.

Pharmacodynamic properties

Mitexan is an antidote, and offers the possibility of reliably preventing urotoxic side- effects associated with aggressive cancer chemotherapy using oxazaphosphorine cytostatics. Extensive and wide-ranging pharmacological and toxicological investigations have shown that Mitexan has no intrinsic pharmacodynamics and low toxicity. The pharmacological and toxicological inertness of Mitexan administered systemically and its excellent detoxifying effect in the efferent urinary tract and bladder, are due to the nature of its pharmacokinetics.

Pharmacokinetic properties

Mitexan, a free thiol, is easily and rapidly transformed by auto-oxidation into its only metabolite Mitexan-disulphide (diMitexan). DiMitexan remains in the intravascular compartment and is quickly transported to the kidneys.

In the epithelium of renal tubuli, diMitexan is again reduced to the free thiol compound, which is then able to react chemically in the urine with toxic oxazaphosphorine metabolites.

Elimination (being almost exclusively renal) starts immediately after administration. Excretion is as the free thiol (Mitexan) in the first 4 hours after a single dose, and almost exclusively as the disulphide (diMitexan) thereafter. Renal elimination is almost complete after approximately 8 hours.

Approximately 30% of an intravenous dose is bioavailable as free thiol (Mitexan) in the urine.

Name of the medicinal product

Mitexan

Qualitative and quantitative composition

Mesna

Special warnings and precautions for use

WARNINGS

Hypersensitivity

Hypersensitivity reactions to Mitexan have been reported following administration of Mitexan as an uroprotectant. These include various skin and subcutaneous tissue symptoms.

In addition, cases of severe bullous and ulcerative skin and mucosal reactions were reported.

In some cases, skin reactions were accompanied by one or more other symptoms, such as fever, cardiovascular symptoms, pulmonary symptoms, haematological abnormalities, nausea, vomiting, pain in the extremities, arthralgia, myalgia, malaise, and conjunctivitis.

Some reactions have presented as anaphylaxis.

Fever accompanied by, e.g., hypotension but no skin manifestations has also been reported.

Some patients with a history of a reaction have shown positive delayed-type skin test results. However, a negative delayed reaction does not exclude hypersensitivity to Mitexan. Positive immediate-type skin test reactions have occurred in patients regardless of previous Mitexan exposure or history of hypersensitivity reactions, and may be related to the concentration of the Mitexan solution used for testing.

Prescribers should be aware that:

- severe as well as minor reactions were reported with the use of Mitexan in regimens to treat both severe systemic autoimmune disease and malignancy and that Mitexan should be suspected in any hypersensitivity reaction,

- these reactions may occur with first exposure or after several months of exposure and in some cases can be life threatening,

- the occurrence and severity of reactions appeared to vary with the dose administered with a tendency to shorter intervals following subsequent exposures,

- hypersensitivity reactions to Mitexan were interpreted to resemble the clinical picture of sepsis and, in patients with autoimmune disorders, resemble an exacerbation of the underlying disease.

ThiolCompounds:

Mitexan is a thiol compound, i.e., a sulfhydryl (SH) group-containing organic compound. Thiol compounds show some similarities in their adverse reaction profile, including a potential to elicit severe skin reactions. Examples of drugs that are thiol compounds include amifostine, penicillamine, and captopril.

It is not clear whether patients who experienced an adverse reaction to such a drug are at increased risk for any reactions, or similar reactions, to another thiol compound. However, when considering subsequent use of another thiol compound in such patients, the possibility of an increased risk should be taken into account.

PRECAUTIONS

Mitexan does not prevent hemorrhagic cystitis in all patients. Patients should be monitored accordingly.

Sufficient urinary output should be maintained, as required for oxazaphosphorine treatment.

Sodium content

Mitexan solution for injection contains approximately 59 mg of sodium per 400 mg Mitexan.

Lab test interferences

Mitexan treatment may cause false positive reactions in nitroprusside sodium-based urine tests (including dipstick tests) for ketone bodies.

Effects on ability to drive and use machines

Patients undergoing treatment with Mitexan may experience undesirable effects (including, e.g., syncope, light-headedness, lethargy/drowsiness, dizziness, and blurred vision) which could affect the ability to drive or use machines. The decision to drive or operate machinery should be made on an individual basis.

Dosage (Posology) and method of administration

Sufficient Mitexan must be given to adequately protect the patient from the urotoxic effects of the oxazaphosphorine.

The duration of Mitexan treatment should equal that of the oxazaphosphorine treatment plus the time taken for the urinary concentration of oxazaphosphorine metabolites to fall to non-toxic levels. This usually occurs within 8-12 hours after the end of oxazaphosphorine treatment but may vary depending on the scheduling of oxazaphosphorine. Urinary output should be maintained at 100 ml/hr (as required for oxazaphosphorine treatment) and the urine monitored for haematuria and proteinuria throughout the treatment period.

Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration.

Any solutions which are discolored, hazy, or contain visible particulate matter should not be used.

Where ifosfamide or cyclophosphamide is used as an iv bolus: Mitexan is given by intravenous injection over 15-30 minutes at 20% of the simultaneously administered oxazaphosphorine on a weight for weight basis (w/w). The same dose of Mitexan is repeated after 4 and 8 hours. The total dose of Mitexan is 60% (w/w) of the oxazaphosphorine dose. This is repeated on each occasion that the cytotoxic agents are used.

Example dosage schedule:

0 hrs

4 hrs

8 hrs

Cyclophosphamide/Ifosfamide

2 g

-

-

Mitexan

400 mg

400 mg

400 mg

If necessary the dose of Mitexan can be increased to 40% of the oxazaphosphorine dose given four times at three hourly intervals (0, 3, 6 and 9 hours). (Total dose = 160% (w/w) of the oxazaphosphorine dose). This larger dose is recommended in children, in patients whose urothelium may be damaged from previous treatment with oxazaphosphorine or pelvic irradiation, or in patients who are not adequately protected by the standard dose of Mitexan.

Example dosage schedule:

0 hrs

3 hrs

6 hrs

9 hrs

Cyclophosphamide/Ifosfamide

2 g

-

-

Mitexan

800 mg

800 mg

800 mg

800 mg

Where cyclophosphamide is used orally: The same dose regimen of Mitexan applies as though cyclophosphamide were used as an i.v. bolus.

Where ifosfamide is used as a 24-hour infusion: Mitexan can be used as a concurrent infusion. An initial 20% (w/w) of the total ifosfamide dose is given as an i.v. bolus, then an infusion of 100% (w/w) of the ifosfamide over 24 hours, followed by a further 12-hour infusion of 60% (w/w) of the ifosfamide dose. Total Mitexan dose = 180% of the ifosfamide dose.

Example dosage schedule:

0 hrs

0-24 hrs

24 hrs

28 hrs

32 hrs

36 hrs

Ifosfamide

-

5 g/m2 infusion

-

-

-

-

Mitexan

1 g/m 2 iv

5 g/m2 infusion

3g/m2 infusion

1 g/m2 iv

1 g/m2 iv

1 g/m2 iv

Where ifosfamide is used as a long-term infusion:

An initial 20% (w/w) of the first 24 hours ifosfamide dose is given as an i.v. bolus as the ifosfamide infusion starts. Then each 24 hour infusion of ifosfamide is given with a concurrent 24 hour infusion (100% w/w) of Mitexan. A 12 hour infusion of Mitexan (60% (w/w) of the final 24 hour dose of ifosfamide) should be commenced as the ifosfamide-Mitexan infusion finishes.

Example dosage schedule:

Day 1

Day 2

Day 3

Day 4

0 hrs

0-24 hrs

0-24 hrs

0-24 hrs

24 hrs

4 hrs

8 hrs

12 hrs

Ifosfamide

-

2 g/m2 infusion

2 g/m2 infusion

2 g/m2 infusion

-

-

-

-

Mitexan

0.4g/m2 iv

2 g/m2 infusion

2 g/m2 infusion

2 g/m2 infusion

1.2 g/m2 infusion

0.4 g/m2 iv

0.4 g/m2 iv

0.4 g/m2 iv

The final 12-hour infusion of Mitexan, after long-term or 24 hour infusion of ifosfamide, may be replaced by boluses at 28, 32 and 36 hours, each of 20% (w/w) of the ifosfamide dose, or by oral Mitexan.

Mitexan can be mixed in the same infusion bag as the ifosfamide.

Oral use of Mitexan ampoules: Mitexan has been shown to be effective when taken orally. Compared with intravenous administration, overall availability of Mitexan in urine after oral administration is approximately 50%; the onset of urinary excretion is delayed by up to 2 hours and is more prolonged than following intravenous dosing.

With the exception of continuous long-term infusions of oxazaphosphorines with Mitexan, intravenously administered Mitexan may be replaced by oral administration of Mitexan. The dosage should be 40% w/w of the dosage of the oxazaphosphorines. The contents of the ampoule should be added to a flavoured soft drink (e.g. orange juice, cola). This mixture is stable when refrigerated in a sealed container for 24 hours.

For intermittent oxazaphosphorine therapy following an initial intravenous injection of Mitexan at a dose of 20% (w/w) of the oxazaphosphorine dose, oral Mitexan (40% w/w) should be administered at 2 hours and again at 6 hours after the initial intravenous dose. Alternatively, three oral doses of Mitexan may be administered, replacing the i.v. dose with an oral dose (40% w/w) 2 hours prior to administration of oxazaphosphorines.

Example dosage schedule:

- 2 hrs

0 hrs

2 hrs

6 hrs

Cyclophosphamide/Ifosfamide

-

1 g iv

-

-

Mitexan

400 mg po

-

400 mg po

400 mg po

200 mg iv

400 mg po

400 mg po

Where ifosfamide is used as a long-term continuous infusion with concomitant Mitexan, oral Mitexan may be taken as the infusion of ifosfamide and Mitexan finishes, then at 2 hours and 6 hours after the time at the finish of the infusion. All oral Mitexan doses should be 40% (w/w) of the final 24 hour ifosfamide dose.

Example dosage schedule:

0 hrs

0-24 hrs

24 hrs

26 hrs

30 hrs

Ifosfamide

-

5 g/m2 infusion

-

-

-

Mitexan

1 g/m2 iv

5 g/m2 infusion

2 g/m2 po

2 g/m2 po

2 g/m2 po

Mitexan is also available for oral administration as Mitexan Tablets. For further information see the Summary of Product Characteristics for Mitexan Tablets or contact Baxter Healthcare Limited.

Children

Children generally micturate more frequently than adults and therefore it may be necessary to shorten the interval between doses and/or to increase the number of individual doses.

Elderly

No specific information is available. Clinical trials have included patients over 65 and no adverse reactions specific to this age group have been reported.

Special precautions for disposal and other handling

No special instructions necessary.