Thiotepa Injection
SUMMARY OF PRODUCT CHARACTERISTICS
1 NAME OF THE MEDICINAL PRODUCT
Thiotepa Injection
2 QUALITATIVE AND QUANTITATIVE COMPOSITION
Thiotepa 15mg
3 PHARMACEUTICAL FORM
Sterile powder for injection
4 CLINICAL PARTICULARS
4.1 Therapeutic indications
Thiotepa (N,N',N" triethylenethiophosphoramide) is a polyfunctional alkylating agent used alone or in combination with other cytotoxic drugs, or with surgery in the treatment of neoplastic diseases. It is believed to exert its cytotoxic effects by the alkylation of DNA.
4.2 Posology and method of administration
Thiotepa (15mg) should be reconstituted with 1.5ml Water for Injection immediately prior to use. Please refer to specific sections on particular disease types for further reconstitution instructions. Reconstituted solutions should be clear to slightly opaque. Solutions that are grossly opaque or precipitated should be discarded.
Use Luer-Lock fittings on all syringes and sets. Large bore needles are recommended to minimise pressure and possible formation of aerosols. The latter may also be reduced by the use of a venting needle.
Thiotepa may be given by intravenous, intramuscular and intrathecal routes of injection; it may be given directly into pleural, pericardial or peritoneal cavities and as a bladder instillation.
Since absorption from the gastrointestinal tract is variable, Thiotepa should not be administered orally.
Dosage must be carefully individualised. A slow response to Thiotepa does not necessarily indicate a lack of effect. Therefore, increasing the frequency of dosing may only increase toxicity.
For intramuscular injection, bladder and intracavitary instillations:
Dosage: Adults, Adolescents over 12 years and the elderly
Up to 60mg in single or divided doses. Doses should be reduced in cases of leucopenia as indicated in Table 1. Single dose administration of 90mg Thiotepa as a bladder instillation is described under "Bladder Cancer".
Table 1
|
WBC Count 3 Cells/mm |
Dose of Thiotepa Adults and Adolescents over 12 years |
|
6000 |
60mg |
|
5000 - 6000 |
45mg |
|
4500 - 5000 |
30mg |
|
4000 - 4500 |
20mg |
|
3500 - 4000 |
10mg |
|
3000 - 3500 |
5mg |
|
below 3000 |
omit dose |
Children: Use in children is not recommended.
Intrathecal injection: Up to a maximum of 10mg.
It is essential that a complete blood count should be performed 12-24 hours before each dose of Thiotepa. Thrombocytopenia in the absence of leucopenia has been noted.
Dosage schedules of Thiotepa vary widely according to the route of administration and the indication.
Examples of dosage schedules used according to specific tumour types are given below:
Breast Cancer:
Patients with advanced breast cancer have been treated with Thiotepa as part of a combination regime, given intramuscularly in divided doses of 15-30mg three times weekly for two weeks; this representing one course of treatment. An interval of six to eight weeks is recommended between courses to allow bone marrow recovery.
An alternative schedule employs Thiotepa as part of a combination regime, given as an initial priming dose of 15mg intramuscularly or intravenously each day for four days. This may be followed in three weeks by maintenance doses of 15mg I.M. every 14-21 days.
Bladder Cancer:
Instillations of Thiotepa have been used to treat multiple superficial tumours of the bladder, resulting in a complete clinical response in about one third of patients. Patients are dehydrated for 8-12 hours prior to treatment. Up to 60mg Thiotepa dissolved in 60ml sterile water is instilled into the bladder by catheter once a week for four weeks. During removal of the catheter following instillation, Thiotepa injection is continued to ensure bathing of the prostatic and pendulous urethra. The solution should be retained for up to two hours and the patient should be frequently repositioned to ensure maximum contact with the urothelium.
Patients are generally cystoscoped two weeks after a course of four instillations. If a response is observed a second course of four Thiotepa instillations may be given, generally at a reduced dosage, e.g. 15-60mg with intervals of one to two weeks between instillations.
Second and third courses must be given with caution since bone-marrow depression may be increased. Deaths have occurred after intravesical administration, caused by bone-marrow depression from systemically absorbed drug.
Instillations of Thiotepa have been used prophylactically as an adjunct to surgical resection of superficial tumours of the bladder, resulting in a marked decrease in the recurrence rate. It is recommended that there should be a minimum interval of one week between tumour resection and the commencement of prophylactic instillation of Thiotepa. 30-60mg Thiotepa dissolved in 60ml sterile water is instilled into the bladder for two hours and repeated at intervals of one to two weeks for a total of 4-8 instillations. This initial course may be followed by instillations of Thiotepa, 30-60mg every four to six weeks for one year or longer.
Single dose Thiotepa instillations have been used prophylactically as an adjunct of surgical resection in the treatment of superficial tumours of the bladder. 90mg Thiotepa dissolved in 100mg sterile water is instilled into the bladder with the patient in the left lateral position. After 15 minutes the patient is transferred to the right lateral position and after a further 15 minutes the bladder is emptied. It is felt that such single dose administration may decrease the incidence of systemic toxicity by decreasing the extent of systemic absorption of the drug.
Note: Patients who have had previous radiotherapy to the bladder are at increased risk of drug toxicity.
Malignant meningeal disease:
Intrathecal injections of Thiotepa have been found to be useful for the palliative treatment of cases of meningeal infiltration by leukaemia and lymphoma. Clinical experience has shown Thiotepa to be effective in carcinomatous involvement of the meninges, but published data is limited. Thiotepa, at a concentration of 1mg/ml in sterile water, is administered by injection through a lumbar theca, in doses of up to 10mg on alternate days until there is clearance of malignant cells from the cerebrospinal fluid (CSF). It is recommended that if no improvement occurs in the CSF after three injections, then treatment should be changed. Not more than four injections should be given on alternative days. Routine blood counts should be performed prior to each dose of Thiotepa.
Ovarian cancer:
Ovarian cancer has been treated with Thiotepa as a single agent or as part of a combination regime in a variety of schedules. For example, 15mg Thiotepa I.V. or I.M. may be given daily for four days initially and then continued with single doses administered once a week or once every two weeks.
Intracavitary instillation of Thiotepa:
Instillations of Thiotepa have been used to treat malignant pleural effusions and abdominal ascites. The procedure recommended, is first to aspirate as much fluid as possible and then to instil the dose of Thiotepa, 10-60mg in 20-60ml sterile water. This may be repeated once a week or once every two weeks.
Prevention of recurrences of Pterygium:
A 1:2,000 solution of Thiotepa in sterile Ringer's solution (i.e. 15mg powder in 30ml Ringer's), applied topically as eye drops, every three hours daily for up to six weeks after surgical removal of the pterygium, is effective in reducing the recurrence rate following surgery.
Condyloma Acuminata:
Thiotepa applied topically or instilled intraurethrally in a gel, has been successfully used to eradicate condyloma acuminata. The drug may be administered by first reconstituting 60mg Thiotepa with 5ml sterile water. This is diluted to 15ml, using a sterile mixture of water and lubricating jelly made to a consistency viscous enough to remain in the urethra and fluid enough to allow easy injection. This therapy may be repeated at weekly intervals.
4.3 Contraindications
Thiotepa administration is contra-indicated in patients with a WBC count below 3,000 and/or a platelet count below 100,000 and in patients with known hypersensitivity to ingredients of this preparation.
4.4 Special warnings and precautions for use
Death from septicaemia and haemorrhage has occurred as a direct result of haematopoietic depression by Thiotepa. Death has also occurred after intravesical administration, caused by bone-marrow depression from systemically absorbed drug.
Thiotepa is highly toxic to the haematopoietic system. WBC and platelet counts are recommended 12-24 hours before each dose of Thiotepa, at weekly intervals during therapy, and for at least three weeks after therapy has been discontinued, regardless of route of administration, except when used topically as eye drops or in the treatment of condyloma acuminata. Bone marrow depression may be delayed; the nadir in blood cell and platelet counts may occur up to 30 days after treatment is stopped. Myelosuppression has occasionally been prolonged.
Dosage should be adjusted according to WBC count (see table 1, section 4.2 Posology and Method of Administration). Thiotepa administration is contraindicated in patients with WBC count below 3,000 and/or a platelet count below 100,000 (see section 4.3 Contra-indications). Treatment should be discontinued if the white cell or platelet count falls rapidly.
Thiotepa should be used with extreme caution in general not be used in patients with existing hepatic, renal or bone marrow damage and only if the need outweighs the risk in such patients. The lowest effective dosage should be used and careful monitoring is recommended. with hepatic, renal and haematopoietic function tests.
In general, dose selection for an elderly patient should be cautious, usually starting at the low end of the dosing range, reflecting the greater frequency of decreasing hepatic, renal or cardiac function, and of concomitant disease or other drug therapy.
Safe use in children has not been established.
Effective contraception should be used during Thiotepa therapy if either the patient or the partner is of childbearing potential.
Thiotepa should only be used by clinicians who are familiar with the various characteristics of cytotoxic drugs and their clinical toxicity.
Thiotepa must be stored in a refrigerator (2-8°C). The occurrence of a precipitate on reconstitution (with 1.5ml of Water for Injection) indicates that polymerisation has occurred with the formation of less active constituents and the injection must be discarded.
Reconstituted solutions may be stored in a refrigerator (2-8 °C) for 24 hours. However, if a precipitate forms, the solution must be discarded.
Thiotepa may be mixed in the same syringe with procaine hydrochloride 2% or with adrenaline 1 in 1,000 or with both.
Trained personnel should reconstitute Thiotepa in a designated area. Caution should be exercised in handling and preparation of Thiotepa. Adequate protective gloves and goggles should be worn and the work surface should be covered with plastic-backed absorbent paper. Thiotepa is not a vesicant and should not cause harm if it comes in contact with the skin. It should, of course, be washed off with water immediately. If Thiotepa contacts mucous membranes, the membranes should be flushed thoroughly with water. Any transient stinging may be treated with bland cream. The cytotoxic preparation should not be handled by pregnant staff.
Any spillage or waste material may be disposed of by incineration. We do not make any specific recommendations with regard to the temperature of the incinerator.
Thiotepa has been reported to possess mutagenic activity on the basis of bacterial, plant and mammalian mutagenicity tests. It has also been reported to be carcinogenic in mice and rats. These effects are consistent with its activity as an alkylating agent. There is some evidence of carcinogenicity in man. In patients treated with Thiotepa, cases of myelodysplastic syndromes and acute non-lymphocytic leukaemia have been reported.
4.5 Interaction with other medicinal products and other forms of interaction
It is not advisable to combine, simultaneously or sequentially, cancer chemotherapeutic agents or a cancer chemotherapeutic agent and a therapeutic modality having the same mechanism of action. Therefore, Thiotepa combined with other alkylating agents such as nitrogen mustard or cyclophosphamide or Thiotepa combined with irradiation would serve to intensify toxicity rather than to enhance therapeutic response. If these agents must follow each other, it is important that recovery from the first agent, as indicated by white blood cell count, be complete before therapy with the second agent is instituted.
Other drugs which are known to produce bone-marrow depression should be avoided.
Thiotepa enhances effects of suxamethonium.
Cytotoxics reduce absorption of digoxin tablets.
Cytotoxics possibly reduce absorption of phenytoin.
4.6 Fertility, pregnancy and lactation
Thiotepa can cause foetal harm when administered to a pregnant woman.
Thiotepa is teratogenic and embryotoxic in mice and rats following intraperitoneal administration. In addition, it has been reported to interfere with spermatogenesis and ovarian function in rodent species.
There are no adequate and well-controlled studies in pregnant women. Patients of childbearing potential should be advised to avoid pregnancy. The drug therefore, should not normally be administered to patients who are pregnant or to mothers who are breast feeding unless the benefit outweighs the risk to foetus or child.
If Thiotepa is used during pregnancy, or if pregnancy occurs during Thiotepa therapy, the patient and partner should be apprised of the potential hazard to the foetus.
There are no data on the excretion of Thiotepa in human breast milk. Breast feeding should be discontinued during and for three months following the use of Thiotepa.
4.7 Effects on ability to drive and use machines
None
4.8 Undesirable effects
The most serious side-effect is upon the blood forming elements and is a direct consequence of the cytotoxic effect of the drug. Death from septicaemia and haemorrhage has occurred as a direct consequence of haematopoietic suppression.
Infections and Infestations Increased susceptibility to infections.
Neoplasms benign and malignant (including cysts and polyps)
Myelodysplastic syndrome, acute non-lymphocytic leukemia.
Blood and lymphatic system disorders
Bone marrow depression, thrombocytopenia, haematopoietic suppression. Thromboembolism-Venous thromboembolism can be a complication of cancer itself, but chemotherapy can also increase the risk.
Immune system disorders Allergic reactions.
Metabolism and nutrition disorders
Anorexia
Nervous system disorders Headache, dizziness.
Eye disorders
Depigmentation of periorbital skin after using Thiotepa eye drops, blurred vision, conjunctivitis.
Gastrointestinal disorders
Nausea, vomiting, diarrhoea, abdominal pain. Oral mucositis- A sore mouth is a common complication of cancer chemotherapy.
Skin and subcutaneous tissue disorders Rash, contact dermatitis, alopecia.
Renal and urinary disorders
Haemorrhagic cystitis after intravesical or intravenous administration, dysuria, urinary retention.
Reproductive system and breast disorders
Impairment of fertility, amenorrhoea, interference with spermatogenesis. General disorders and administration site conditions
Fatigue, weakness, febrile reaction, pain at injection site, skin discolouration following topical use or exposure, local irritation comparable to mild radiation cystitis following bladder instillations.
A number of cytotoxic drugs will cause severe local tissue necrosis if leakage into the extravascular compartment occurs. To reduce the risk of extravasation injury it is recommended that cytotoxic drugs are administered by appropriately trained staff.
Tumour lysis syndrome
Tumour lysis syndrome can occur secondary to spontaneous or treatment related rapid destruction of malignant cells. Features include hyperkalaemia, hyperuricaemia and hyperphosphataemia with hypocalcaemia; renal damage and arrhythmias can follow.
4.9 Overdose
Manifestations of overdose are primarily reflections of the decreased blood cell and platelet counts due to haematopoietic toxicity, which may become life-threatening. Bleeding due to low platelet counts may occur, and the patient is more vulnerable to, and less able to combat infections.
There is no specific antidote. General supportive measures are recommended. Thiotepa may be removed using dialysis. Blood counts should be carried out to estimate damage to the haematopoietic system. Whole blood, platelet, or leucocyte transfusions have proven beneficial.
PHARMACOLOGICAL PROPERTIES
5.
5.1. Pharmacodynamic Properties
Thiotepa is an ethyleneimine compound whose antineoplastic effect is related to its alkylating action. It is not a vesicant and may be given by all parenteral routes, as well as directly into tumour masses.
5.2. Pharmacokinetic Properties
Variable absorption occurs from intramuscular injection sites. Absorption through serous membranes such as the bladder and pleura occurs to some extent. Only traces of unchanged Thiotepa and triethylene phosphoramide are excreted in the urine, together with a large proportion of metabolites.
5.3. Pre-clinical Safety Data
Thiotepa has been shown to be mutagenic in various in vitro assays, and carcinogenic in animal studies.
Studies in animals have shown Thiotepa to impair spermatogenesis and ovarian function.
6. PHARMACEUTICAL PARTICULARS 6.1. List of Excipients
Water for Injection
6.2. Incompatibilities
None.
6.3. Shelf-Life
18 months.
Special Precautions for Storage
6.4.
Thiotepa must be stored in a refrigerator (2-8°C). Reconstituted solutions may be stored in a refrigerator (2-8°C) for up to 24 hours.
6.5. Nature and Content of Container
Flint glass vial with butyl rubber stopper. Pack Size: 15mg
6.6. Instruction for Use, Handling and Disposal
See” Special Warnings and Precautions”.
7 MARKETING AUTHORISATION HOLDER
Mercury Pharmaceuticals Ltd
Capital House
85 King William Street
London
EC4N 7BL
UK
8 MARKETING AUTHORISATION NUMBER(S)
PL 12762/0159
9 DATE OF FIRST AUTHORISATION/RENEWAL OF THE AUTHORISATION
22/08/1991
DATE OF REVISION OF THE TEXT
31/03/2014
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