KIT FOR THE PREPARATION OF TECHNETIUM TC99M SESTAMIBI (tetrakis(2-methoxyisobutylisocyanide)copper- i tetrafluoroborate injection, powder, lyophilized, for solution

Kit for the Preparation of Technetium Tc99m Sestamibi by

Drug Labeling and Warnings

Kit for the Preparation of Technetium Tc99m Sestamibi by is a Prescription medication manufactured, distributed, or labeled by Lantheus Medical Imaging, Inc., Jubilant HollisterStier LLC. Drug facts, warnings, and ingredients follow.

Drug Details [pdf]

  • 1. INDICATIONS AND USAGE

    Myocardial Imaging: Technetium Tc99m Sestamibi is a myocardial perfusion agent that is indicated for detecting coronary artery disease by localizing myocardial ischemia (reversible defects) and infarction (non-reversible defects), in evaluating myocardial function and developing information for use in patient management decisions. Technetium Tc99m Sestamibi evaluation of myocardial ischemia can be accomplished with rest and cardiovascular stress techniques (e.g., exercise or pharmacologic stress in accordance with the pharmacologic stress agent's labeling).

    It is usually not possible to determine the age of a myocardial infarction or to differentiate a recent myocardial infarction from ischemia.

    Breast Imaging: Technetium Tc99m Sestamibi is indicated for planar imaging as a second line diagnostic drug after mammography to assist in the evaluation of breast lesions in patients with an abnormal mammogram or a palpable breast mass.

    Technetium Tc99m Sestamibi is not indicated for breast cancer screening, to confirm the presence or absence of malignancy, and it is not an alternative to biopsy.

  • 2. DOSAGE AND ADMINISTRATION

    For Myocardial Imaging: The suggested dose range for I.V. administration of Technetium Tc99m Sestamibi in a single dose to be employed in the average patient (70 Kg) is 370-1110 MBq (10-30 mCi).

    For Breast Imaging: The recommended dose range for I.V. administration of Technetium Tc99m Sestamibi is a single dose of 740-1110 MBq (20 - 30 mCi).

    2.1 Image Acquisition

    Breast Imaging: It is recommended that images are obtained with a table overlay to separate breast tissue from the myocardium and liver, and to exclude potential activity that may be present in the opposite breast. For lateral images, position the patient prone with the isolateral arm comfortably above the head, shoulders flat against the table, head turned to the side and relaxed, with the breast imaged pendent through an overlay cutout. The breast should not be compressed on the overlay. For anterior images, position the patient supine with both arms behind the head. For either lateral or anterior images, shield the chest and abdominal organs, or remove them from the field of view.

    For complete study, sets of images should be obtained five minutes after the injection, and in the following sequence:

    Beginning five minutes after the injection of Technetium Tc99m Sestamibi:

    • ten-minute lateral image of breast with abnormality
    • ten-minute lateral image of contralateral breast
    • ten-minute anterior image of both breasts

    2.2 Radiation Dosimetry

    The radiation doses to organs and tissues of an average patient (70 Kg) per 1110 MBq (30 mCi) of Technetium Tc99m Sestamibi injected intravenously are shown in Table 1.0.

    Table 1.0. Radiation Absorbed Doses from Tc99m Sestamibi
    Estimated Radiation Absorbed Dose
    REST
    2.0 hour void4.8 hour void
    Organrads/30 mCimGy/1110 MBqrads/30 mCimGy/1110 MBq
    Breasts0.22.00.21.9
    Gallbladder Wall2.020.02.020.0
    Small Intestine3.030.03.030.0
    Upper Large Intestine Wall5.455.55.455.5
    Lower Large Intestine Wall3.940.04.241.1
    Stomach Wall0.66.10.65.8
    Heart Wall0.55.10.54.9
    Kidneys2.020.02.020.0
    Liver0.65.80.65.7
    Lungs0.32.80.32.7
    Bone Surfaces0.76.80.76.4
    Thyroid0.77.00.77.0
    Ovaries1.515.51.615.5
    Testes0.33.40.43.9
    Red Marrow0.55.10.55.0
    Urinary Bladder Wall2.020.04.241.1
    Total Body0.54.80.54.8
    STRESS
    2.0 hour void4.8 hour void
    Organrads/30 mCimGy/1110 MBqrads/30 mCimGy/1110 MBq
    Breasts0.22.00.21.8
    Gallbladder Wall2.828.92.827.8
    Small Intestine2.424.42.424.4
    Upper Large Intestine Wall4.544.44.544.4
    Lower Large Intestine Wall3.332.23.332.2
    Stomach Wall0.65.30.55.2
    Heart Wall0.55.60.55.3
    Kidneys1.716.71.716.7
    Liver0.44.20.44.1
    Lungs0.32.60.22.4
    Bone Surfaces0.66.20.66.0
    Thyroid0.32.70.22.4
    Ovaries1.212.21.313.3
    Testes0.33.10.33.4
    Red Marrow0.54.60.54.4
    Urinary Bladder Wall1.515.53.030.0
    Total Body0.44.20.44.2

    Radiation dosimetry calculations performed by Radiation Internal Dose Information Center, Oak Ridge Institute for Science and Education, PO Box 117, Oak Ridge, TN 37831-0117.

    2.3 Instructions For Preparation

    Preparation of the Technetium Tc99m Sestamibi is done by the following aseptic procedure:

    General Procedure:

    • a. Prior to adding the Sodium Pertechnetate Tc99m Injection to the vial, inspect the vial carefully for the presence of damage, particularly cracks, and do not use the vial if found. Tear off a radiation symbol and attach it to the neck of the vial.
    • b. Waterproof gloves should be worn during the preparation procedure. Remove the plastic disc from the vial and swab the top of the vial closure with alcohol to sanitize the surface.

    Boiling Water Bath Procedure:

    • c. Place the vial in a suitable radiation shield with a fitted radiation cap.
    • d. With a sterile shielded syringe, aseptically obtain additive-free, sterile, non-pyrogenic Sodium Pertechnetate Tc99m Injection [925-5550 MBq, (25-150 mCi)] in approximately 1 to 3 mL.
    • e. Aseptically add the Sodium Pertechnetate Tc99m Injection to the vial in the lead shield. Without withdrawing the needle, remove an equal volume of headspace to maintain atmospheric pressure within the vial.
    • f. Shake vigorously, about 5 to 10 quick upward-downward motions.
    • g. Remove the vial from the lead shield and place upright in an appropriately shielded and contained boiling water bath, such that the vial is suspended above the bottom of the bath, and boil for 10 minutes. Timing for 10 minutes is begun as soon as the water begins to boil again. Do not allow the boiling water to come in contact with the aluminum crimp.
    • h. Remove the vial from the water bath, place in the lead shield and allow to cool for fifteen minutes.

    Recon-o-Stat (thermal cycler) Procedure:

    • c. Place the vial in the thermal cycler radiation shield.
    • d. With a sterile shielded syringe, aseptically obtain additive-free, sterile, non-pyrogenic Sodium Pertechnetate Tc99m Injection [925-5550 MBq, (25-150 mCi)] in approximately 1 to 3 mL.
    • e. Aseptically add the Sodium Pertechnetate Tc99m Injection to the vial in the lead shield. Without withdrawing the needle, remove an equal volume of headspace to maintain atmospheric pressure within the vial.
    • f. Shake vigorously, about 5 to 10 quick upward-downward motions.
    • g. Place shield on sample block. While slightly pressing downward, give the shield a quarter turn to make certain there is a firm fit between the shield and the sample block.
    • h. Press the proceed button to initiate the program (the thermal cycler automatically heats & cools the vial and contents). Please see the Recon-o-Stat Instruction Manual for further details.

    General Procedure (cont.):

    • i. Using proper shielding, the vial contents should be visually inspected. Use only if the solution is clear and free of particulate matter and discoloration.
    • j. Assay the reaction vial using a suitable radioactivity calibration system. Record the Technetium Tc99m concentration, total volume, assay time and date, expiration time and lot number on the vial shield label and affix the label to the shield.
    • k. Store the reaction vial containing the Technetium Tc99m Sestamibi at 15° to 25°C until use; at such time the product should be aseptically withdrawn. Technetium Tc99m Sestamibi should be used within six hours of preparation. The vial contains no preservative.

    Note: Adherence to the above product reconstitution instructions is recommended.

    The potential for cracking and significant contamination exists whenever vials containing radioactive material are heated.

    Product should be used within 6 hours after preparation.

    Final product with radiochemical purity of at least 90% was used in the clinical trials that established safety and effectiveness. The radiochemical purity was determined by the following method.

    2.4 Determination of Radiochemical Purity in Technetium Tc99m Sestamibi

    1. Obtain a Baker-Flex Aluminum Oxide coated, plastic TLC plate, #1 B-F, pre-cut to 2.5 cm × 7.5 cm.
    2. Dry the plate or plates at 100°C for 1 hour and store in a desiccator. Remove pre-dried plate from the desiccator just prior to use.
    3. Apply 1 drop of ethanol1 using a 1 mL syringe with a 22-26 gauge needle, 1.5 cm from the bottom of the plate. THE SPOT SHOULD NOT BE ALLOWED TO DRY.
    4. Add 2 drops of Technetium Tc99m Sestamibi solution, side by side on top of the ethanol1 spot. Return the plate to a desiccator and allow the sample spot to dry (typically 15 minutes).
    5. The TLC tank is prepared by pouring ethanol1 to a depth of 3-4 mm. Cover the tank and let it equilibrate for ~10 minutes.
    6. Develop the plate in the covered TLC tank in ethanol1 for a distance of 5 cm from the point of application.
    7. Cut the TLC plate 4 cm from the bottom and measure the Tc99m activity in each piece by appropriate radiation detector.
    8. Calculate the % Tc99m Sestamibi as:
      % Tc99m Sestamibi =µCi Top Piece   
      µCi Both Pieces
      × 100
    Figure 1 TLC Plate Diagram
    Figure 1

  • 1 The ethanol used in this procedure should be 95% or greater. Absolute ethanol (99%) should remain at ≥ 95% ethanol content for one week after opening if stored tightly capped, in a cool dry place.
  • 3. DOSAGE FORMS AND STRENGTHS

    Kit for the Preparation of Technetium Tc99m Sestamibi for Injection is supplied as a lyophilized mixture in a 5 mL vial.

  • 4. CONTRAINDICATIONS

    None known.

  • 5. WARNINGS AND PRECAUTIONS

    5.1 Warnings

    In studying patients in whom cardiac disease is known or suspected, care should be taken to assure continuous monitoring and treatment in accordance with safe, accepted clinical procedure. Infrequently, death has occurred 4 to 24 hours after Tc99m Sestamibi use and is usually associated with exercise stress testing (See Section 5.2).

    Pharmacologic induction of cardiovascular stress may be associated with serious adverse events such as myocardial infarction, arrhythmia, hypotension, bronchoconstriction and cerebrovascular events. Caution should be used when pharmacologic stress is selected as an alternative to exercise; it should be used when indicated and in accordance with the pharmacologic stress agent's labeling.

    Technetium Tc99m Sestamibi has been rarely associated with acute severe allergic and anaphylactic events of angioedema and generalized urticaria. In some patients the allergic symptoms developed on the second injection during Technetium Tc99m Sestamibi imaging. Caution should be exercised and emergency equipment should be available when administering Technetium Tc99m Sestamibi. Also, before administering Technetium Tc99m Sestamibi patients should be asked about the possibility of allergic reactions to the drug.

    5.2 General Precautions

    The contents of the vial are intended only for use in the preparation of Technetium Tc99m Sestamibi and are not to be administered directly to the patient without first undergoing the preparative procedure.

    Radioactive drugs must be handled with care and appropriate safety measures should be used to minimize radiation exposure to clinical personnel. Also, care should be taken to minimize radiation exposure to the patients consistent with proper patient management.

    Contents of the kit before preparation are not radioactive. However, after the Sodium Pertechnetate Tc99m Injection is added, adequate shielding of the final preparation must be maintained. The components of the kit are sterile and non-pyrogenic. It is essential to follow directions carefully and to adhere to strict aseptic procedures during preparation.

    Technetium Tc99m labeling reactions depend on maintaining the stannous ion in the reduced state. Hence, Sodium Pertechnetate Tc99m Injection containing oxidants should not be used.

    Technetium Tc99m Sestamibi should not be used more than six hours after preparation.

    Radiopharmaceuticals should be used only by physicians who are qualified by training and experience in the safe use and handling of radionuclides and whose experience and training have been approved by the appropriate government agency authorized to license the use of radionuclides.

    Stress testing should be performed only under the supervision of a qualified physician and in a laboratory equipped with appropriate resuscitation and support apparatus.

    The most frequent exercise stress test endpoints sufficient to stop the test reported during controlled studies (two-thirds were cardiac patients) were:

    Fatigue35%
    Dyspnea17%
    Chest Pain16%
    ST-depression7%
    Arrhythmia1%
  • 6. ADVERSE REACTIONS

    Adverse events were evaluated in 3741 adults who were evaluated in clinical studies. Of these patients, 3068 (77% men, 22% women, and 0.7% of the patient's genders were not recorded) were in cardiac clinical trials and 673 (100% women) in breast imaging trials. Cases of angina, chest pain, and death have occurred (see Section 5). Adverse events reported at a rate of 0.5% or greater after receiving Technetium Tc99m Sestamibi administration are shown in the following table:

    Table 2.0 Selected Adverse Events Reported in > 0.5% of Patients Who Received Technetium Tc99m Sestamibi in Either Breast or Cardiac Clinical Studies*
    Body SystemBreast StudiesCardiac Studies
    Women
    n = 673
    Women
    n = 685
    Men
    n = 2361
    Total
    n = 3046
  • * Excludes the 22 patients whose gender were not recorded.
  • Body as a Whole21 (3.1%)6 (0.9%)17 (0.7%)23 (0.8%)
      Headache11 (1.6%)2 (0.3%)4 (0.2%)6 (0.2%)
    Cardiovascular9 (1.3%)24 (3.5%)75 (3.2%)99 (3.3%)
      Chest Pain/Angina0 (0%)18 (2.6%)46 (1.9%)64 (2.1%)
      ST segment changes0 (0%)11 (1.6%)29 (1.2%)40 (1.3%)
    Digestive System8 (1.2%)4 (0.6%)9 (0.4%)13 (0.4%)
      Nausea4 (0.6%)1 (0.1%)2 (0.1%)3 (0.1%)
    Special Senses132 (19.6%)62 (9.1%)160 (6.8%)222 (7.3%)
      Taste Perversion129 (19.2%)60 (8.8%)157 (6.6%)217 (7.1%)
      Parosmia8 (1.2%)6 (0.9%)10 (0.4%)16 (0.5%)

    In the clinical studies for breast imaging, breast pain was reported in 12 (1.7%) of the patients. In 11 of these patients the pain appears to be associated with biopsy/surgical procedures.

    The following adverse reactions have been reported in ≤ 0.5% of patients: signs and symptoms consistent with seizure occurring shortly after administration of the agent; transient arthritis, angioedema, arrythmia, dizziness, syncope, abdominal pain, vomiting, and severe hypersensitivity characterized by dyspnea, hypotension, bradycardia, asthenia, and vomiting within two hours after a second injection of Technetium Tc99m Sestamibi. A few cases of flushing, edema, injection site inflammation, dry mouth, fever, pruritis, rash, urticaria and fatigue have also been attributed to administration of the agent.

  • 7. DRUG INTERACTIONS

    Specific drug-drug interactions have not been studied.

  • 8. USE IN SPECIFIC PATIENTS

    8.1 Pregnancy

    Animal reproduction and teratogenicity studies have not been conducted with Technetium Tc99m Sestamibi. It is also not known whether Technetium Tc99m Sestamibi can cause fetal harm when administered to a pregnant woman or can affect reproductive capacity. There have been no studies in pregnant women. Technetium Tc99m Sestamibi should be given to a pregnant woman only if clearly needed.

    8.3 Nursing Mothers

    Technetium Tc99m Pertechnetate is excreted in human milk during lactation. It is not known whether Technetium Tc99m Sestamibi is excreted in human milk. Therefore, formula feedings should be substituted for breast feedings.

    8.4 Pediatric Use

    Safety and effectiveness in the pediatric population have not been established.

    No evidence of diagnostic efficacy or clinical utility of Technetium Tc99m Sestamibi scan was found in clinical studies of children and adolescents with Kawasaki disease.

    A prospective study of 445 pediatric patients with Kawasaki disease was designed to determine the predictive value of Technetium Tc99m Sestamibi rest and stress myocardial perfusion imaging to define a pediatric population with Kawasaki disease that was at risk of developing cardiac events. Cardiac events were defined as cardiac death, MI, hospitalization due to cardiac etiology, heart failure, CABG or coronary angioplasty. The standard of truth was defined as cardiac events occurring 6 months following the administration of Technetium Tc99m Sestamibi. Only three cardiac events were observed at six months in this study. In all three cases, the scan was negative. No clinically meaningful measurements of sensitivity, specificity or other diagnostic performance parameters could be demonstrated in this study.

    A ten year retrospective case history study of pediatric Kawasaki disease patients who completed Technetium Tc99m Sestamibi myocardial perfusion imaging and who had coronary angiography within three months of the Technetium Tc99m Sestamibi scan was designed to measure sensitivity and specificity of Technetium Tc99m Sestamibi scan. Out of 72 patients who had both evaluable Technetium Tc99m Sestamibi scans and evaluable angiographic images, only one patient had both an abnormal angiogram and an abnormal Technetium Tc99m Sestamibi scan. No clinically meaningful measurements of sensitivity, specificity or other diagnostic performance parameters could be demonstrated in this study.

    In a clinical pharmacology study, 46 pediatric patients with Kawasaki disease received Technetium Tc99m Sestamibi administration at the following doses: 0.1-0.2 mCi/kg for rest, 0.3 mCi/kg for stress in one day studies; 0.2 mCi/kg for rest and 0.2 mCi/kg for stress in two day studies.

    The radioactivity both in younger children and in adolescents exhibited PK profiles similar to those previously reported in adults (See Section 12).

    The radiation absorbed doses in adolescents, both at rest and stress, were similar to those observed in adults (see Section 2). When comparing weight-adjusted radioactivity (up to 0.3 mCi/kg) doses administered to adolescents and younger children to the recommended dose administered to adults (up to 30 mCi ), the radiation absorbed doses in both adolescents and younger children were similar to those in adults.

    Adverse events were evaluated in 609 pediatric patients from the three clinical studies described above. The frequency and the type of the adverse events were similar to the ones observed in the studies of Technetium Tc99m Sestamibi in adults. Two of the 609 had a serious adverse event: one patient received a Technetium Tc99m Sestamibi overdose but remained asymptomatic, and one patient had an asthma exacerbation following administration.

    8.5 Geriatric Use

    In two separate clinical studies: Of 3068 patients in clinical studies of Technetium Tc99m Sestamibi, 693 patients were 65 or older and 121 were 75 or older.

    Of 673 patients in clinical studies of Technetium Tc99m Sestamibi, 138 patients were 65 or older and 30 were 75 or older.

    Based on the evaluation of the frequency of adverse events and review of vital signs data, no overall differences in safety were observed between these subjects and younger subjects. Although reported clinical experience has not identified differences in response between elderly and younger patients, greater sensitivity of some older individuals cannot be ruled out.

  • 9. DRUG ABUSE AND DEPENDENCE

    9.1 Controlled Substance

    Not applicable.

    9.2 Abuse

    Not applicable.

    9.3 Dependence

    Not applicable.

  • 10. OVERDOSAGE

    The clinical consequences of overdosing with Technetium Tc99m Sestamibi are not known.

  • 11. DESCRIPTION

    Each 5 mL vial contains a sterile, non-pyrogenic, lyophilized mixture of:

    • Tetrakis (2-methoxy isobutyl isonitrile) Copper (I) tetrafluoroborate - 1.0 mg
    • Sodium Citrate Dihydrate - 2.6 mg
    • L-Cysteine Hydrochloride Monohydrate - 1.0 mg
    • Mannitol – 20 mg
    • Stannous Chloride, Dihydrate, minimum (SnCl2∙2H2O) - 0.025 mg
    • Stannous Chloride, Dihydrate, (SnCl2∙2H2O) - 0.075 mg
    • Tin Chloride (stannous and stannic) Dihydrate, maximum (as SnCl2∙2H2O) - 0.086 mg

    Prior to lyophilization the pH is 5.3 to 5.9. The contents of the vial are lyophilized and stored under nitrogen.

    This drug is administered by intravenous injection for diagnostic use after reconstitution with sterile, non-pyrogenic, oxidant-free Sodium Pertechnetate Tc99m Injection. The pH of the reconstituted product is 5.5 (5.0 - 6.0). No bacteriostatic preservative is present.

    The precise structure of the technetium complex is Tc99m[MIBI]6+ where MIBI is 2-methoxy isobutyl isonitrile.

    11.1 Physical Characteristics

    Technetium Tc99m decays by isomeric transition with a physical half-life of 6.02 hours2. Photons that are useful for detection and imaging studies are listed below in Table 3.0.

    Table 3.0. Principal Radiation Emission Data
    RadiationMean %/DisintegrationMean Energy (KeV)
    Gamma -289.07140.5

  • 2 Kocher, David, C., Radioactive Decay Data Tables, DOE/TIC-11026, 108(1981).
  • 11.2 External Radiation

    The specific gamma ray constant for Tc99m is 5.4 microcoulombs/Kg-MBq-hr (0.78R/mCi-hr) at 1 cm. The first half value layer is 0.017 cm of Pb. A range of values for the relative attenuation of the radiation emitted by this radionuclide that results from interposition of various thicknesses of Pb is shown in Table 4.0. To facilitate control of the radiation exposure from Megabequerel (millicurie) amounts of this radionuclide, the use of a 0.25 cm thickness of Pb will attenuate the radiation emitted by a factor of 1,000.

    Table 4.0. Radiation Attenuation by Lead Shielding
    Shield Thickness (Pb) cmCoefficient of Attenuation
    0.0170.5
    0.0810-1
    0.1610-2
    0.2510-3
    0.3310-4

    To correct for physical decay of this radionuclide, the fractions that remain at selected intervals after the time of calibration are shown in Table 5.0.

    Table 5.0 Physical Decay Chart; Tc99m Half-Life 6.02 Hours
    Hours Fraction RemainingHours Fraction Remaining
  • * Calibration Time
  • 0*1.0008.398
    1.8919.355
    2.79410.316
    3.70811.282
    4.63112.251
    5.562
    6.501
    7.447
  • 12. CLINICAL PHARMACOLOGY

    12.1 Mechanism of Action

    Technetium Tc99m Sestamibi is a cationic Tc99m complex which has been found to accumulate in viable myocardial tissue in a manner analogous to that of thallous chloride Tl-201. Scintigraphic images obtained in humans after the intravenous administration of the drug have been comparable to those obtained with thallous chloride Tl-201 in normal and abnormal myocardial tissue.

    Animal studies have shown that myocardial uptake is not blocked when the sodium pump mechanism is inhibited. Although studies of subcellular fractionation and electron micrographic analysis of heart cell aggregates suggest that Tc99m Sestamibi cellular retention occurs specifically within the mitochondria as a result of electrostatic interactions, the clinical relevance of these findings has not been determined.

    The mechanism of Tc99m Sestamibi localization in various types of breast tissue (e.g., benign, inflammatory, malignant, fibrous) has not been established.

    12.3 Pharmacokinetics

    Pulmonary activity is negligible even immediately after injection. Blood clearance studies indicate that the fast clearing component clears with a t1/2 of 4.3 minutes at rest, and clears with a t1/2 of 1.6 minutes under exercise conditions. At five minutes post injection about 8% of the injected dose remains in circulation. There is less than 1% protein binding of Technetium Tc99m Sestamibi in plasma. The myocardial biological half-life is approximately six hours after a rest or exercise injection. The biological half-life for the liver is approximately 30 minutes after a rest or exercise injection. The effective half-life of clearance (which includes both the biological half-life and radionuclide decay) for the heart is approximately 3 hours, and for the liver is approximately 30 minutes, after a rest or exercise injection. The ideal imaging time reflects the best compromise between heart count rate and surrounding organ uptake.

    Myocardial uptake which is coronary flow dependent is 1.2% of the injected dose at rest and 1.5% of the injected dose at exercise. Table 6.0 illustrates the biological clearance as well as effective clearance (which includes biological clearance and radionuclide decay) of Tc99m Sestamibi from the heart and liver.

    [Organ concentrations expressed as percentage of injected dose; data based on an average of 5 subjects at rest and 5 subjects during exercise].

    Table 6.0 Biological and Effective Clearance
    RESTSTRESS
    HeartLiverHeartLiver
    TimeBiologicalEffectiveBiologicalEffectiveBiologicalEffectiveBiologicalEffective
    5 min.1.21.219.619.41.51.55.95.8
    30 min.1.11.012.211.51.41.34.54.2
    1 hour1.00.95.65.01.41.22.42.1
    2 hours1.00.82.21.71.21.00.90.7
    4 hours0.80.50.70.41.00.60.30.2

    A study in a dog myocardial ischemia model reported that Technetium Tc99m Sestamibi undergoes myocardial distribution (redistribution), although more slowly and less completely than thallous chloride Tl-201. A study in a dog myocardial infarction model reported that the drug showed no redistribution of any consequence. Definitive human studies to demonstrate possible redistribution have not been reported. In patients with documented myocardial infarction, imaging revealed the infarct up to four hours post dose.

    12.3.1 Metabolism

    The agent is excreted without any evidence of metabolism.

    12.3.2 Elimination

    The major pathway for clearance of Tc99m Sestamibi is the hepatobiliary system. Activity from the gall bladder appears in the intestines within one hour of injection. Twenty-seven percent of the injected dose is excreted in the urine, and approximately thirty-three percent of the injected dose is cleared through the feces in 48 hours.

  • 13. NONCLINICAL TOXICOLOGY

    13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility

    In comparison with most other diagnostic technetium labeled radiopharmaceuticals, the radiation dose to the ovaries (1.5 rads/30 mCi at rest, 1.2 rads/30 mCi at exercise) is high. Minimal exposure (ALARA) is necessary in women of childbearing capability. (See Section 2.)

    The active intermediate, Cu(MIBI)4BF4, was evaluated for genotoxic potential in a battery of five tests. No genotoxic activity was observed in the Ames, CHO/HPRT and sister chromatid exchange tests (all in vitro). At cytotoxic concentrations (> 20 µg/mL), an increase in cells with chromosome aberrations was observed in the in vitro human lymphocyte assay. Cu(MIBI)4BF4 did not show genotoxic effects in the in vivo mouse micronucleus test at a dose which caused systemic and bone marrow toxicity (9 mg/kg, > 600 × maximal human dose).

  • 14. CLINICAL STUDIES

    CLINICAL TRIALS:

    MYOCARDIAL IMAGING: In a trial of rest and stress Technetium Tc99m Sestamibi imaging, the relationship of normal or abnormal perfusion scans and long term cardiac events was evaluated in 521 patients (511 men, 10 women) with stable chest pain. There were 73.9% Caucasians, 25.9% Blacks and 0.2% Asians. The mean age was 59.6 years (range: 29 to 84 years). All patients had a baseline rest and exercise Technetium Tc99m Sestamibi scan and were followed for 13.2 ± 4.9 months (range: 1 to 24 months). Images were correlated with the occurrence of a cardiac event (cardiac death or non-fatal myocardial infarction). In this trial as summarized in Table 7.0, 24/521 (4.6%) had a cardiac event.

    Table 7.0 Cardiac Events
    Baseline Scan*Proportion of patients with events by scan results *Proportion of scan result in patients with events;
    N=24*
    Proportion of event-free patients by scan result *
  • * Note: Similar findings were found in two studies with patients who had pharmacologic stress Technetium Tc99m Sestamibi imaging.
  • p<0.01
  • Normal1/206 (0.5%)1/24 (4.2%)205/206 (99.5%)
    Abnormal23/315 (7.3%) 23/24 (95.8%) 292/315 (92.7%)

    Although patients with normal images had a lower cardiac event rate than those with abnormal images, in all patients with abnormal images it was not possible to predict which patient would be likely to have further cardiac events; i.e., such individuals were not distinguishable from other patients with abnormal images.

    The findings were not evaluated for defect location, disease duration, specific vessel involvement or intervening management.

    In earlier trials, using a template consisting of the anterior wall, inferior-posterior wall and isolated apex, localization in the anterior or inferior-posterior wall in patients with suspected angina or coronary artery disease was shown. Disease localization isolated to the apex has not been established. In adults, Tc99m Sestamibi has not been studied or evaluated in cardiac disorders other than coronary artery disease.

    BREAST IMAGING: Technetium Tc99m Sestamibi was evaluated in two multicenter, clinical trials of a total of 673 woman patients. Overall the mean age was 52 (range 23 to 87 years). The racial and ethnic representation was 70% Caucasian, 15% African-American, 14% Hispanic and 1% Asian.

    Both clinical studies evaluated women who were referred for further evaluation for either: 1) a mammographically detected (with varying degrees of malignant likelihood) but not palpable breast lesion (study A, n=387, mean age = 54 years), or 2) a palpable breast lesion (study B, n=286, mean age = 50 years). In both studies all patients were scheduled for biopsy.

    Technetium Tc99m Sestamibi (20-30 mCi) was injected intravenously in a vein that was contralateral to the breast lesion in question. Planar imaging was completed with a high resolution collimator with a 10% window centered at 140 KeV, and 128 × 128 matrix. An initial marker image, that was not used in the data analysis, was obtained using a cobalt Co57 point source as a marker of a palpable mass. Images were obtained 5 minutes after injection as follows: lateral image of the affected breast for 10 minutes, lateral image of the contralateral breast for 10 minutes, and an anterior image of both breasts for 10 minutes. For the lateral image the patients were positioned in a prone position. For the anterior image, the patients were supine. The Technetium Tc99m Sestamibi scintigraphic images were read in a randomized method by two groups of three blinded readers. Technetium Tc99m Sestamibi uptake was scored as: normal (no uptake), equivocal, low, moderate, or high uptake. The results of Technetium Tc99m Sestamibi images and mammography were analyzed in comparison to histopathologic findings of malignant or non-malignant disease.

    As shown in Table 8.0 for the 483 evaluable patients, the sensitivity and specificity of any degree of Technetium Tc99m Sestamibi uptake appear to vary with the presence or absence of palpable mass.

    TABLE 8.0 Overall Technetium Tc99m Sestamibi Blinded Results of Target Lesions* Identified at Study Entry
    STATISTICStudy A Non-Palpable Mass and an Abnormal MammogramStudy B Palpable Mass
    Number of Patients and LesionsN=277 Patients with 300 LesionsN=206 Patients with 240 Lesions
  • * Excludes all discordant lesions not identified at entry and excludes 25 equivocal interpretations from Study A and 32 equivocal interpretations from Study B (see Tables 9.0 and 10.0)
  • Some patients had more than one target lesion
  • Median and approximated 95% Confidence Interval
  • § PPV= Positive Predict Value; NPV= Negative Predict Value
  • Sensitivity52(42,62)76(67,83)
    Specificity94(89,96)85(77,91)
    PPV§79(67,88)83(74,89)
    NPV§80(74,85)78(69,84)
    Agreement80(75,85)80(75,85)
    Prevalence32(27,37)49(43,56)

    In a separate retrospective subset analyses of 259 patients with dense (heterogeneously/extremely dense) and 275 patients with fatty (almost entirely fat/numerous vague densities) breast tissue, the Technetium Tc99m Sestamibi results were similar. Overall, the studies were not designed to compare the performance of Technetium Tc99m Sestamibi with the performance of mammography in patients with breast densities or other coexistent breast tissue disorders.

    In general the histology seems to correlate with the degree of Technetium Tc99m Sestamibi uptake. As shown in Tables 9.0 and 10.0, the majority of the normal Technetium Tc99m Sestamibi images are associated with non-malignant tissue (78-81%) and the majority of low, moderate or high uptake Technetium Tc99m Sestamibi images are associated with malignant disease (79-83%). In an individual patient, however, the intensity of Technetium Tc99m Sestamibi uptake can not be used to confirm the presence or absence of malignancy. Equivocal results do not have a correlation with histology.

    TABLE 9.0 Degree of Technetium Tc99m Sestamibi Breast Imaging Uptake in Comparison to Histopathology Results in Patients with Mammographically Detected Non-Palpable Lesions* (Study A)
    Normal Uptake
    N = 249 lesions
    Equivocal Uptake
    N = 25 lesions
    Low, Moderate or High Uptake
    N = 66 lesions
  • * Median finding for 3 blinded readers
  • Includes benign tissue, fibroadenoma, benign intramammary nodes, radial scar.
  • Non-malignant201 (81%)14 (56%)14 (21%)
    Malignant48 (19%)11 (44%)52 (79%)
    TABLE 10.0 Degree of Technetium Tc99m Sestamibi Breast Imaging Uptake in Comparison to Histopathology Results in Patients with Palpable Lesions* (Study B)
    Normal Uptake
    N = 129 lesions
    Equivocal Uptake
    N = 32 lesions
    Low, Moderate or High Uptake
    N = 115 lesions
  • * Median finding for 3 blinded readers
  • Includes benign tissue, fibroadenoma, benign intramammary nodes, radial scar.
  • Non-malignant100 (78%)19 (59%)20 (17%)
    Malignant29 (22%)13 (41%)95 (83%)

    An estimate of the likelihood of malignancy based on the Technetium Tc99m Sestamibi uptake score in combination with the mammographic score has not been studied.

    In these two studies approximately 150 additional, non-biopsied lesions were found to be positive after Technetium Tc99m Sestamibi imaging. These lesions were identified in sites that did not physically correlate with identified entry criteria mammographic lesions and these lesions were not palpable. These lesions were not biopsied. Whether these lesions were benign or malignant is not known. Technetium Tc99m Sestamibi uptake can occur in both benign and malignant disease. THE CLINICAL USEFULNESS OF A POSITIVE TECHNETIUM Tc99M SESTAMIBI IMAGE IN THE ABSENCE OF AN ABNORMAL MAMMOGRAM OR A PALPABLE LESION IS NOT KNOWN.

  • 15. REFERENCES

    Not applicable.

  • 16. HOW SUPPLIED/STORAGE AND HANDLING

    Kit for the Preparation of Technetium Tc99m Sestamibi for Injection is supplied as a 5 mL vial in a kit of twenty (20) vials (NDC # 11994-003-20), sterile and non-pyrogenic.

    The patient dose should be measured by a suitable radioactivity calibration system immediately prior to patient administration. Radiochemical purity should be checked prior to patient administration.

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

    Store at 15-25°C (59-77°F) before and after reconstitution.

    Prior to lyophilization the pH is between 5.3 and 5.9. The contents of the vial are lyophilized and stored under nitrogen. Store at 15-25°C (59-77°F) before and after reconstitution. Technetium Tc99m Sestamibi contains no preservatives. Included in each twenty (20) vial kit is one (1) package insert, twenty four (24) vial shield labels and twenty four (24) radiation warning labels.

    This reagent kit is approved for distribution to persons licensed pursuant to the Code of Massachusetts Regulations 105 CMR 120.500 for the uses listed in 105 CMR 120.547 or 120.552, or under equivalent regulations of the U.S. Nuclear Regulatory Commission, Agreement States or Licensing States.

  • 17. PATIENT COUNSELING INFORMATION

    Patients should be advised to inform their health care provider if they had an allergic reaction to Technetium Tc99m Sestamibi or if they had an imaging study with Technetium Tc99m Sestamibi.

  • SPL UNCLASSIFIED SECTION

    Distributed by:
    Lantheus Medical Imaging
    331 Treble Cove Road
    N. Billerica, Massachusetts 01862 USA
    For Ordering Tel: Toll Free 800-229-3431
    All Other Business: 800-362-2668
    (For Massachusetts and International call 978-667-9531)

    515927-0514

  • PRINCIPAL DISPLAY PANEL - 5 mL Vial Kit Box

    Reorder #: GNCA

    Kit for the Preparation of
    Technetium Tc99m Sestamibi
    for Injection

    Rx only

    WARNING: Radiopharmaceuticals should be used by persons who are qualified by specific training in the
    safe use and handling of radionuclides and whose experience and training have been approved
    by the appropriate governmental agency authorized to license the use of radionuclides.

    PRINCIPAL DISPLAY PANEL - 5 mL Vial Kit Box
  • INGREDIENTS AND APPEARANCE
    KIT FOR THE PREPARATION OF TECHNETIUM TC99M SESTAMIBI 
    tetrakis(2-methoxyisobutylisocyanide)copper(i) tetrafluoroborate injection, powder, lyophilized, for solution
    Product Information
    Product TypeHUMAN PRESCRIPTION DRUGItem Code (Source)NDC: 11994-003
    Route of AdministrationINTRAVENOUS
    Active Ingredient/Active Moiety
    Ingredient NameBasis of StrengthStrength
    TETRAKIS(2-METHOXYISOBUTYLISOCYANIDE)COPPER(I) TETRAFLUOROBORATE (UNII: N6OU7HJ70P) (TETRAKIS(2-METHOXYISOBUTYLISOCYANIDE)COPPER(I) TETRAFLUOROBORATE - UNII:N6OU7HJ70P) TETRAKIS(2-METHOXYISOBUTYLISOCYANIDE)COPPER(I) TETRAFLUOROBORATE1 mg  in 1 mL
    Inactive Ingredients
    Ingredient NameStrength
    TRISODIUM CITRATE DIHYDRATE (UNII: B22547B95K) 2.6 mg  in 1 mL
    CYSTEINE HYDROCHLORIDE (UNII: ZT934N0X4W) 1 mg  in 1 mL
    MANNITOL (UNII: 3OWL53L36A) 20 mg  in 1 mL
    STANNOUS CHLORIDE (UNII: 1BQV3749L5) 0.075 mg  in 1 mL
    Packaging
    #Item CodePackage DescriptionMarketing Start DateMarketing End Date
    1NDC: 11994-003-2020 in 1 BOX12/20/1990
    15 mL in 1 VIAL; Type 0: Not a Combination Product
    Marketing Information
    Marketing CategoryApplication Number or Monograph CitationMarketing Start DateMarketing End Date
    NDANDA01978512/20/1990
    Labeler - Lantheus Medical Imaging, Inc. (176786812)
    Establishment
    NameAddressID/FEIBusiness Operations
    Lantheus Medical Imaging, Inc.176786812RELABEL(11994-003) , REPACK(11994-003) , MANUFACTURE(11994-003) , LABEL(11994-003) , PACK(11994-003) , ANALYSIS(11994-003)
    Establishment
    NameAddressID/FEIBusiness Operations
    Jubilant HollisterStier LLC069263643MANUFACTURE(11994-003) , ANALYSIS(11994-003)

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