Summary of medicine characteristics - IOMERON 300 SOLUTION FOR INJECTION
1 NAME OF THE MEDICINAL PRODUCT
1 NAME OF THE MEDICINAL PRODUCTIomeron 300, solution for injection
2. Qualitative and quantitative composition
Contains 61.24% w/v of concentration of iomeprol equivalent to 30% iodine or 300mg iodine/ml.
For excipients, see 6.1.
3. Pharmaceutical form
3. Pharmaceutical formSolution for injection
4. CLINICAL PARTICULARS
4.1. Therapeutic indications
X-ray contrast medium used for: peripheral arteriography venography
angiogardiography and left ventriculography cerebral arteriography
visceral arteriography
digital subtraction angiography computed tomography enhancement urography
ERCP
dacryocystography
sialography
fistulography galactography myelography
4.2 Posology and method of administration
| peripheral arteriography | adults children | 10 – 90ml 1 * 1 |
| venography | adults | 10 – 100ml1 max 250ml 10 – 50ml upper extremity 50 – 100ml lower extremity |
| angiocardiography and left | adults | 30 – 80ml max 250ml |
| ventriculography | children | * 1 |
| cerebral arteriography | adults children | 5 – 12ml 1 3 – 7ml or 1 1 |
| visceral arteriography | adults children | 5 – 50ml1 or according to type of examination; max 250ml * 1 |
| digital subtraction angiography intra arterial | ||
| visceral | adults | 2 – 20ml per artery1 aorta 25–50ml1 both 250ml max |
| peripheral | adults | 5 – 10ml per artery1 max 250ml |
| intravenous | adults | 30 – 60ml1 max 250ml |
| computed tomography | ||
| brain | adults children | 50 – 150ml * 1 |
| body | adults children | 40 – 150ml max 250ml * 1 |
| urography intravenous | adults neonates babies children | 50 – 150ml 3 – 4.8ml/kg 2.5 – 4ml 1 – 2.5ml/kg or 1 |
| arthrography | adults | 1 – 10ml |
| ERCP | adults | 12 – 30ml |
| dacryocystography | adults | 3 – 8ml |
| sialography | adults | 1 – 3ml |
| fistulography | adults | 1 – 50ml |
| galactography | adults | 0.2 – 1.5ml |
| myelography | adults | 10 – 15ml by lumbar injection |
In myelography, lower doses may be used for lumbar or thoracic studies and higher doses for cervical or total columnar studies. Regardless of the nature of the myelographic study, Iomeron should be injected slowly over 1–2 minutes.
The X ray can be taken up to 60 minutes following injection. Post myelographic CT of the spinal column should be delayed for approximately four hours to allow dilution and clearance of excessive contrast.
4.3 Contraindications
Hypersensitivity to the active substance or any of the excipients.
Intrathecal concomitant administration of corticosteroids with contrast media is contraindicated.
4.4 Special warnings and special precautions for use
In consideration of possible complications, the patient should be kept under observation for at least 30 minutes after the examination.
Extreme caution during injection of contrast media is necessary to avoid extravasation.
Hydration
Patients must be well hydrated, and any relevant abnormalities of fluid or electrolyte balance should be corrected prior to and following contrast media injection. Especially patients with diabetes mellitus, polyuria, oligouria, hyperuricaemia, infants, small children, and elderly patients, should not be exposed to dehydration. Also patients with severely compromised hepatic and renal impairment are more at risk. Caution should be exercised in hydrating patients with underlying conditions that may be worsened by fluid overload, including congestive heart failure.
Rehydration prior to use of iomeprol is recommended in patients with sickle cell disease.
Special population
Hypersensitivity to iodinated contrast media, allergic predisposition
A positive history of allergy, asthma or untoward reaction during previous similar investigations indicates a need for extra caution since, as with other contrast media, this product may provoke anaphylaxis or other manifestations of allergy with nausea, vomiting, dyspnoea, erythema, urticaria and hypotension. The benefits should clearly outweigh the risks in such patients and appropriate resuscitative measures should be immediately available. The primary treatments are as follows:
| Effect | Major Symptoms | Primary Treatment |
| Vasomotor effect | warmth nausea/vomiting | reassurance |
| Cutaneous | scattered hives severe urticaria | H1 -antihistamines H2 -antihistamines |
| Bronchospastic | wheezing | oxygen Beta-2-agonist inhalers |
| Anaphylactoid | angioedema | oxygen |
| reaction | urticaria bronchospasm | iv fluids adrenergics (iv epinephrine) |
hypotension
Inhaled beta-2-adrenergics
antihistamines (H1-and
H2– blockers) corticosteroids
Hypotensive hypotension iv fluids
Vagal reaction hypotension iv fluids
bradycardia iv atropine
From: Bush WH; The Contrast Media Manual; Katzburg RW Ed.; Williams and Wilkins; Baltimore 1992; Chapter 2 p 23
The risk of bronchospasm-inducing reactions in asthmatic patients is higher after contrast media administration, especially in patients taking beta-blockers.
Hypersensitivity testing
In patients with suspected or known hypersensitivity to contrast media, sensitivity test doses are not recommended, as severe or fatal reactions to contrast media are not predictable from sensitivity test.
Myelomatosis or paraproteinaemias are conditions predisposing to renal impairment following CM administration. The benefits of the use of a contrast-enhanced procedure should be carefully weighted against the possible risk. Adequate hydration and monitoring of renal function are recommended after CM administration.
Cardiovascular diseases
Care should be taken in severe cardiac disease particularly heart failure and coronary artery disease. Reactions may include pulmonary oedema, haemodynamic changes, ischaemic ECG changes and arrhythmias. In severe, chronic hypertension the risk of renal damage following administration of a contrast medium is increased. In these cases the risks associated with the catheterization procedure are increased.
The product should be used with caution in patients with hyperthyroidism or goitre. Use may interfere with thyroid function tests.
The administration of iodinated contrast media may aggravate myasthenia signs and symptoms.
CNS Disorders
Particular care is needed in patients with acute cerebral infarction, acute intracranial haemorrhage and any conditions involving damage to the blood brain barrier, brain oedema or acute demyelination. Convulsive seizures are more likely in patients with intracranial tumours or metastases or with a history of epilepsy.
Neurological symptoms related to cerebrovascular diseases, intracranial tumours/metastases or degenerative or inflammatory pathologies may be exacerbated.
There is an increased risk of transient neurological complications in patients with symptomatic cerebrovascular disease eg stroke, transient ischaemic attacks. Cerebral ischaemic phenomena may be caused by intravascular injection.
Anticonvulsant therapy should not be discontinued
In acute and chronic alcoholism the increase in blood brain barrier permeability facilitates the passage of the contrast medium into cerebral tissue possibly leading to CNS disorders. There is a possibility of a reduced seizure threshold in alcoholics.
In patients with a drug addiction there is also the possibility of a reduced seizure threshold.
Patients with phaeochromocytoma may develop severe, occasionally uncontrollable hypertensive crises during intra-arterial administration. Premedication with an alpha and beta receptor blocker is recommended in these patients. Pronounced excitement, anxiety and pain can cause side effects or intensify reaction to the contrast medium. A sedative may be given.
Renal impairment
In patients with moderate to severe impairment of renal function, attention should be paid to renal function parameters before re-examining the patient with a contrast media.
Preventive measures include:
– identification of high-risk patients;
– ensuring adequate hydration before CM administration, preferably by maintaining i.v. infusion before and during the procedure and until the CM has been cleared by the kidneys;
avoiding whenever possible, the administration of nephrotoxic drugs or major surgery or procedure such as renal angioplasty, until the CM has been cleared;
A combination of severe hepatic and renal impairment delays excretion of the contrast medium therefore such patients should not be examined unless absolutely necessary.
Diabetes mellitus
Care should be taken in renal impairment and diabetes. In these patients it is important to maintain hydration in order to minimise deterioration in renal function.
The presence of renal damage in diabetic patients is one of the factors predisposing to renal impairment following contrast media administration. This may precipitate lactic acidosis in patients who are taking metformin (see section 4.5 – Interaction with medicaments and other forms of interaction)..
Children: Infants up to 1 year, especially the new-born, are particularly susceptible to electrolyte imbalance and haemodynamic alterations. Care should be taken regarding the dosage used.
Transient hypothyroidism may occur in neonates when the mother or the neonate has received an iodinated contrast agent. Thyroid function tests (usually TSH and T4) are recommended in neonates 7–10 days and 1 month after exposure to Iomeron especially in preterm neonates.
Elderly: There is special risk of reactions involving the circulatory system such that myocardial ischaemia, major arrhythmias and extrasystoles are more likely to occur. A combination of neurological disturbances and vascular pathologies present a serious complication. The probability of acute renal insufficiencies is higher in these people.
Precautions for dedicated exams
Angiography
Non ionic contrast media have less anticoagulant activity in vitro than ionic media.
Meticulous attention should therefore be paid to angiographic technique. Non ionic media should not be allowed to remain in contact with blood in a syringe, and intravascular catheters should be flushed frequently to minimise the risk of clotting which, rarely, has led to serious thromboembolic complications.
Intravascular administration should be performed if possible with the patient lying down. The patient should be kept in this position and closely observed for at least 30 minutes after the procedure since the majority of severe incidents occur with this time.
Venography
Special care is required when venography is performed in patients with thrombosis, phlebitis, severe ischaemic disease, local infection or a totally obstructed artero-venous system.
4.5 Interaction with other medicaments and other forms of interaction
Use of the product may interfere with tests for thyroid function. Vasopressor agents should not be administered prior to iomeprol.
Treatment with drugs that lower the seizure threshold such as certain neuroleptics (MAO inhibitors, tricyclic antidepressants), analeptics, and anti-emetics and phenotiazine derivatives should be discontinued 48 hours before the examination. Treatment should not be resumed until 24 hours post-procedure.
It has been reported that cardiac and/or hypertensive patients under treatment with diuretics, ACE-inhibitors, and/or beta blocking agents are at higher risk of adverse reactions when administered iodinated contrast media.
Beta-blockers may impair the response to treatment of bronchospasm induced by contrast medium.
Patients with normal renal function can continue to take metformin normally. In diabetic patients with diabetic nephropathy, under treatment with metformin and with moderate renal impairment, metformin should be stopped at the time of, or prior to the procedure and withheld for 48 hours subsequent to the procedure and reinstituted only after renal function has been re-evaluated and found to be normal In emergency patients in whom renal function is either impaired or unknown, the physician shall weigh out risk and benefit of an examination with a contrast medium and take precautions. Metformin should be stopped from time of contrast medium administration. After the procedure the patient should be monitored for signs of lactic acidosis. Metformin should be restarted 48 hours after contrast medium if serum creatinine/eGFR is unchanged from the pre-imaging level.
Epidural and intrathecal corticosteroids should never be concurrently administered when iodinated contrast media are used, because corticosteroids may promote and affect the signs and symptoms of arachnoiditis (see section 4.3 Contraindications).
Allergy-like reactions to contrast media are more frequent and may manifest as delayed reactions in patients treated with immuno-modulators, like Interleukin-2 (IL-2).
4.6 Fertility, pregnancy and lactation
Women of childbearing potential
Appropriate investigations and measures should be taken when exposing women of childbearing potential to any X-ray examination, whether with or without contrast medium.
Pregnancy
Animal studies have not indicated any harmful effects with respect to the course of pregnancy or on the health of the unborn or neonate. The safety of iomeprol in human pregnancy however has not been established. Therefore avoid in pregnancy unless there is no safer alternative.
Since, wherever possible, exposure to radiation should be avoided during pregnancy, the benefits of any X-ray examination, whether with or without contrast material, should for this reason alone be carefully weighed against the possible risk.
Breastfeeding
No human data exist concerning the excretion of iomeprol in breast milk. Animal studies have demonstrated that the excretion of iomeprol in breast milk is similar to that of other contrast agents and that these compounds are only minimally absorbed by the gastrointestinal tract of the young. Adverse effects on the nursing infant are therefore unlikely to occur.
Stopping breastfeeding is unnecessary.
4.7 Effects on ability to drive and use machines
There is no known effect on the ability to drive and operate machines.
After intrathecal administration, it is recommended that the patient should wait 24 hours before driving or operating machinery.
4.8 Undesirable effects
General
The use of iodinated contrast media may cause untoward side effects. They are usually mild to moderate and transient in nature. However, severe and life-threatening reactions sometimes leading to death have been reported. In most cases, reactions occur within minutes of dosing but at times reactions may occur at later time.
Anaphylaxis (anaphylactoid/hypersensitivity reactions) may manifest with various symptoms, and rarely does any one patient develop all the symptoms. Typically, in 1 to 15 min (but rarely after as long as 2 h), the patient complains of feeling abnormal, agitation, flushing, feeling hot, sweating increased, dizziness, increased lacrimation, rhinitis, palpitations, paresthesia, pruritus, sore throat and throat tightness, dysphagia, cough, sneezing, urticaria, erythema, mild localised oedema, angioneurotic oedema and dyspnoea due to glottic/laryngeal/pharyngeal oedema and/or spasm manifesting with wheezing, and bronchospasm.
Nausea, vomiting, abdominal pain, and diarrhoea are also reported.
These reactions, which can occur independently of the dose administered or the route of administration, may represent the first signs of circulatory collapse.
Administration of the contrast medium must be discontinued immediately and, if needed, appropriate specific treatment urgently initiated via venous access.
Severe reactions involving the cardiovascular system, such as vasodilatation, with pronounced hypotension, tachycardia, dyspnoea, agitation, cyanosis and loss of consciousness progressing to respiratory and/or cardiac arrest may result in death. These events can occur rapidly and require full and aggressive cardio-pulmonary resuscitation.
Primary circulatory collapse can occur as the only and/or initial presentation without respiratory symptoms or without other signs or symptoms outlined above.
The adverse reactions reported in clinical trials among 4,903 adult patients and from post-marketing surveillance are represented in the tables below by frequency and classified by MedDRA system organ class.
Within each frequency grouping, adverse reactions are presented in order of decreasing seriousness.
4.8.1 Intravascular administration
Adult patients involved in clinical trials with intravascular administration of Iomeprol were 4,515.
Adults
| System Organ Class | Adverse Reactions | |||
| Clinical Trials | Post-marketing Surveillance | |||
| Com mon (>1/1 00 t o <1/10 ) | Unco mmo n (>1/1 000 to <1/10 0) | Rare (>1/10, 000 to <1/100 0) | Frequency unknown* | |
| Blood and lymphatic system disorders | Thrombocytopeni a, Haemolytic anaemia | |||
| Immune system disorders | Anaphylactoid reaction | |||
| Psychiatric disorders | Anxiety Confusional state | |||
| Nervous system disorders | Head ache Dizzi ness | Presyn cope | Coma Transient ischaemic attack Paralysis Syncope Convulsion Loss of consciousness Dysarthria Paraesthesia Amnesia Somnolence Taste abnormality | |
| Eye disorders | Blindness transient Visual disturbance Conjunctivitis Lacrimation increased Photopsia | |||
| Cardiac disorders | Bradyc ardia Tachyc ardia Extras ystoles | Cardiac arrest Myocardial infarction Cardiac failure Angina pectoris Arrhythmia Ventricular or atrial fibrillation Atrioventricular | ||
| System Organ Class | Adverse Reactions | |||
| Clinical Trials | Post-marketing Surveillance | |||
| Com mon (>1/1 00 t o <1/10 ) | Unco mmo n (>1/1 000 to <1/10 0) | Rare (>1/10, 000 to <1/100 0) | Frequency unknown* | |
| block Palpitations Cyanosis | ||||
| Vascular disorders | Hype rtensi on | Hypote nsion | Circulatory collapse or shock Hot flush Flushing Pallor | |
| Respiratory, thoracic and mediastinal disorders | Dysp noea | Respiratory arrest Acute respiratory distress syndrome (ARDS) Pulmonary oedema Laryngeal oedema Pharyngeal oedema Bronchospasm Asthma Cough Hyperventilation Pharynx discomfort Laryngeal discomfort Rhinitis Dysphonia | ||
| Gastrointestinal disorders | Naus ea Vomi ting | Diarrhoea Abdominal pain Salivary hypersecretion Dysphagia Salivary gland enlargement | ||
| Skin and subcutaneous tissue disorders | Eryth ema Urtic aria | Rash | Acute generalized exanthematous pustulosis Angioedema | |
| System Organ Class | Adverse Reactions | |||
| Clinical Trials | Post-marketing Surveillance | |||
| Com mon (>1/1 00 t o <1/10 ) | Unco mmo n (>1/1 000 to <1/10 0) | Rare (>1/10, 000 to <1/100 0) | Frequency unknown* | |
| Prurit us | Cold sweat Sweating increased | |||
| Musculoskeletal and connective tissue disorder | Back pain | Arthralgia | ||
| Renal and urinary disorders | Renal failure | |||
| General disorders and administration site conditions | Feeli ng hot | Chest pain Inject ion site warm th and pain | Asthen ia Rigors Pyrexi a | Injection site reaction** Coldness local Fatigue Malaise Thirst |
| Investigations | Blood creatin ine increas ed | El ectrocardi ogram ST segment elevation El ectrocardi ogram abnormal | ||
* Since the reactions were not observed during clinical trials with 4515 patients, best estimate is that their relative occurrence is rare ( >1/10,000 to <1/1000).
The most appropriate MedDRA term is used to describe a certain reaction and its symptoms and related conditions.
** Injection site reactions comprise injection site pain and swelling. In the majority of cases they are due to extravasation of contrast medium. These reactions are usually transient and result in recovery without sequelae. Cases of extravasation with inflammation, skin necrosis and even development of compartment syndrome have been reported.
Coronary artery thrombosis and coronary artery embolism have been reported as a complication of coronary catheterization procedures.
Vasospasm and consequent ischaemia have been observed during intra-arterial injections of contrast medium, in particular after coronary and cerebral angiography often procedurally related and possibly triggered by the tip of the catheter or excess catheter pressure.
As with other iodinated contrast media, very rare cases of mucocutaneous syndromes, including Stevens-Johnson syndrome, toxic epidermal necrolysis (Lyell syndrome) and erythema multiforme, have been reported following the administration of Iomeprol injection.
Paediatric patients
There is limited experience with paediatric patients. The clinical trial paediatric safety database comprises 167 patients.
The Iomeprol safety profile is similar in children and adults.
4.8.2 Intrathecal administration
Adults
Adults patients involved in clinical trials with intrathecal administration of Iomeprol were 388.
The most frequently reported adverse reactions following intrathecal administration of Iomeprol are headache, dizziness, nausea, vomiting and back pain. These reactions are usually mild to moderate and transient in nature. Rarely, headache may persist for days. Most side effects occur some hours (3 to 6 hours) after the procedure, due to the distribution of the contrast medium in the CSF circulation from the site of administration to the intravascular space (see section 5.2: Pharmacokinetic properties). Most reactions usually occur within 24 hours after injection.
| System Organ Class | Adverse Reactions | |||
| Clinical Trials | Postmarket ing Surveil lance | |||
| Very com mon (>1/1 0) | Comm on (>1/100 to <1/10) | Uncommo n (>1/1000 to <1/100) | Freque ncy unkno wn* | |
| Immune system disorders | Anaph ylactoi d reactio n | |||
| Nervous system disorders | Heada che | Dizzine ss | Hypoaesth esia Paraesthesi a Paraparesi s Loss of | Epileps y |
| System Organ Class | Adverse Reactions | |||
| Clinical Trials | Postmarket ing Surveil lance | |||
| Very com mon (>1/1 0) | Comm on (>1/100 to <1/10) | Uncommo n (>1/1000 to <1/100) | Freque ncy unkno wn* | |
| consciousn ess Somnolenc e | ||||
| Vascular disorders | Hyperte nsion | Hypotensi on Flushing | ||
| Gastrointestina l disorders | Nausea Vomitin g | |||
| Skin and subcutaneous tissue disorders | Hyperhidr osis Pruritus | Rash | ||
| Musculoskelet al and connective tissue disorder | Back pain Pain in extremit y | Musculosk eletal stiffness Neck pain | ||
| General disorders and administration site conditions | Injectio n site reaction ** | Feeling hot Pyrexia | ||
* Since the reactions were not observed during clinical trials with 388 patients, best estimate is that their relative occurrence is uncommon (> 1/1000 to <1/100.
The most appropriate MedDRA term is used to describe a certain reaction and its symptoms and related conditions. 2
Blood amylase increased is common following ERCP. Very rare cases of pancreatitis have been described.
The reactions reported in cases of arthrography and fistulography usually represent irritative manifestations superimposed on pre-existing conditions of tissue inflammation.
Hypersensitivity reactions are rare, generally mild and in the form of skin reactions. However, the possibility of severe anaphylactoid reactions cannot be excluded.
As with other iodinated contrast media, pelvic pain and malaise may occur after hysterosalpingography.
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 or search for MHRA Yellow Card in the Google Play or Apple App Store
4.9. Overdose
4.9. OverdoseThe effects of overdose on the pulmonary and cardiovascular systems may become life-threatening. Treatment consists of support of the vital functions and prompt use of symptomatic therapy. Iomeprol does not bind to plasma or serum proteins and is therefore dialyzable.
5. PHARMACOLOGICAL PROPERTIES
5.1. Pharmacodynamic properties
Iomeprol is a low osmolality, non-ionic organic molecule with radio-opacity conferred by an iodine content of 49% of the molecular weight. It is formulated for use as an intravascular/intracavitary/intrathecal contrast medium in concentrations of up to 400mg iodine per ml. Even at this concentration the low viscosity allows delivery of high doses through thin catheters.
5.2. Pharmacokinetic properties
The pharmacokinetics of intravascularly administered iomeprol are similar to those of other iodinated contrast media and conform to a two-compartment model with a rapid distribution and a slower elimination phase. In healthy subjects, the mean distribution and elimination half-lives of iomeprol were 0.5 hours and 1.9 hours respectively.
Distribution volume is similar to that of extra cellular fluid. There is no significant serum protein binding and iomeprol is not metabolized.
Elimination is almost exclusively through the kidneys (90% of the dose recovered in the urine within 96 hours of its administration) and is rapid (50% of an intravascularly administered dose within 2 hours).
Following intrathecal administration to animals, iomeprol is completely cleared from the CSF and passes into the plasma compartment.
5.3. Preclinical safety data
5.3. Preclinical safety dataThere are no pre-clinical data of relevance which are additional to those included in other sections of the SPC.
6. PHARMACEUTICAL PARTICULARS
6.1. List of excipients
trometamol
hydrochloric acid water for injection
6.2. Incompatibilities
No other drug should be mixed with the contrast medium.
6.3. Shelf life
Five years
Solutions not used in one examination session must be discarded.
6.4. Special precautions for storage
Store below 30°C Protect from light
6.5 Nature and contents of container
Colourless Type I or Type II glass bottles with rubber/aluminium cap.
Quantities of 20, 30, 50, 75, 100, 150, 200 or 250 ml of solution.
6.6. Instructions for use/handling
Bottles containing contrast media solution are not intended for the withdrawal of multiple doses. The rubber stopper should never be pierced more than once. The use of proper withdrawal cannulas for piercing the stopper and drawing up the contrast medium is recommended.
Before use, examine the product to assure that the container and closure have not been damaged. Do not use this solution if it is discoloured or particulate matter is present.
The contrast medium should be drawn into the syringe until immediately before use. Withdrawal of contrast agents from their containers should be accomplished under aseptic conditions with sterile syringes. Sterile techniques must be used with any spinal puncture or intravascular injection, and with catheters and guidewires. If non-disposable equipment is used, scrupulous care should be taken to prevent residual contamination with traces of cleansing agents.
It is desirable that solutions of contrast media for intravascular and intrathecal use should be at body temperature when injected.
Any residue of contrast medium in the syringe must be discarded. Solutions not used in one examination session or waste material, such as the connecting tubes, should be disposed in accordance with local requirements.
7. MARKETING AUTHORISATION HOLDER
Bracco UK Ltd Magdalen Centre
The Oxford Science Park
Oxford, OX4 4GA United Kingdom
8.