AXUMIN- fluciclovine f-18 injection, solution
Blue Earth Diagnostics
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HIGHLIGHTS OF PRESCRIBING INFORMATIONThese highlights do not include all the information needed to use AXUMIN safely and effectively. See full prescribing information for AXUMIN.
AXUMIN (fluciclovine F 18) injection, for intravenous use Initial U.S. Approval: 2016 INDICATIONS AND USAGEAxumin is a radioactive diagnostic agent indicated for positron emission tomography (PET) imaging in men with suspected prostate cancer recurrence based on elevated blood prostate specific antigen (PSA) levels following prior treatment ( 1). DOSAGE AND ADMINISTRATION
DOSAGE FORMS AND STRENGTHSInjection: clear, colorless solution in a 30 mL or 50 mL multiple-dose vial containing 335 MBq/mL to 8,200 MBq/mL (9 mCi/mL to 221 mCi/mL) fluciclovine F 18 at calibration time and date ( 3). CONTRAINDICATIONSNone ( 4) WARNINGS AND PRECAUTIONSADVERSE REACTIONSMost commonly reported adverse reactions are injection site pain, erythema, and dysgeusia ( 6.1). To report SUSPECTED ADVERSE REACTIONS, contact Blue Earth Diagnostics, Ltd at 1-855-AXUMIN1 (1-855-298-6461) or FDA at 1-800-FDA-1088 orwww.fda.gov/medwatch. See 17 for PATIENT COUNSELING INFORMATION. Revised: 7/2022 |
Axumin is indicated for positron emission tomography (PET) in men with suspected prostate cancer recurrence based on elevated blood prostate specific antigen (PSA) levels following prior treatment.
Axumin is a radioactive drug and should be handled with appropriate safety measures to minimize radiation exposure during administration [see Warnings and Precautions ( 5.3) ]. Use waterproof gloves and effective shielding, including syringe shields, when handling and administering Axumin.
The recommended dose is 370 MBq (10 mCi) administered as an intravenous bolus injection.
Position the patient supine with arms above the head. Begin PET scanning 3 minutes to 5 minutes after completion of the Axumin injection. It is recommended that image acquisition should start from mid-thigh and proceed to the base of the skull. Typical total scan time is between 20 minutes to 30 minutes.
Localization of prostate cancer recurrence in sites typical for prostate cancer recurrence is based on fluciclovine F 18 uptake in comparison with tissue background. For small lesions (less than 1cm in diameter) focal uptake greater than blood pool should be considered suspicious for prostate cancer recurrence. For larger lesions, uptake equal to or greater than bone marrow is considered suspicious for prostate cancer recurrence.
The radiation absorbed doses estimated for adult patients following intravenous injection of Axumin are shown in Table 1. Values were calculated from human biodistribution data using OLINDA/EXM (Organ Level Internal Dose Assessment/Exponential Modeling) software.
The (radiation absorbed) effective dose resulting from the administration of the recommended activity of 370 MBq of Axumin is 8 mSv. For an administered activity of 370 MBq (10 mCi), the highest-magnitude radiation doses are delivered to the pancreas, cardiac wall, and uterine wall: 38 mGy, 19 mGy, and 17 mGy, respectively. If a CT scan is simultaneously performed as part of the PET procedure, exposure to ionizing radiation will increase in an amount dependent on the settings used in the CT acquisition.
Organ/Tissue | Mean Absorbed Dose per Unit Administered Activity (microGy/MBq) |
Adrenal glands | 16 |
Brain | 9 |
Breasts | 14 |
Gallbladder wall | 17 |
Lower large intestine wall | 12 |
Small intestine wall | 13 |
Stomach wall | 14 |
Upper large intestine wall | 13 |
Heart wall | 52 |
Kidneys | 14 |
Liver | 33 |
Lungs | 34 |
Muscle | 11 |
Ovaries | 13 |
Pancreas | 102 |
Red bone marrow | 25 |
Osteogenic cells | 23 |
Skin | 8 |
Spleen | 24 |
Testes | 17 |
Thymus gland | 12 |
Thyroid | 10 |
Urinary bladder wall | 25 |
Uterus | 45 |
Total body | 13 |
Effective dose | 22 (microSv/MBq) |
Injection: supplied as a clear, colorless solution in a 30 mL or 50 mL multiple-dose vial containing 335 MBq/mL to 8,200 MBq/mL (9 mCi/mL to 221 mCi/mL) fluciclovine F 18 at calibration time and date.
Image interpretation errors can occur with Axumin PET imaging. A negative image does not rule out the presence of recurrent prostate cancer and a positive image does not confirm the presence of recurrent prostate cancer. The performance of Axumin seems to be affected by PSA levels [See Clinical Studies ( 14)] . Fluciclovine F 18 uptake is not specific for prostate cancer and may occur with other types of cancer and benign prostatic hypertrophy in primary prostate cancer. Clinical correlation, which may include histopathological evaluation of the suspected recurrence site, is recommended.
Hypersensitivity reactions including anaphylaxis may occur in patients who receive Axumin. Emergency resuscitation equipment and personnel should be immediately available.
Axumin use contributes to a patient's overall long-term cumulative radiation exposure. Long-term cumulative radiation exposure is associated with an increased risk for cancer. Ensure safe handling to minimize radiation exposure to the patient and health care providers [see Dosage and Administration ( 2.1)] .
Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared to rates in the clinical trials of another drug and may not reflect the rates observed in practice. The clinical trial database for Axumin includes data from 877 subjects including 797 males diagnosed with prostate cancer. Most patients received a single administration of Axumin, a small number of subjects (n = 50) received up to five administrations of the drug. The mean administered activity was 370 MBq (range, 163 MBq to 485 MBq).
Adverse reactions were reported in ≤1% of subjects during clinical studies with Axumin. The most common adverse reactions were injection site pain, injection site erythema and dysgeusia.
In case of overdose of Axumin, encourage patients to maintain hydration and to void frequently to minimize radiation exposure.
Axumin contains the fluorine 18 (F 18) labeled synthetic amino acid analog fluciclovine. Fluciclovine F 18 is a radioactive diagnostic agent used with PET imaging. Chemically, fluciclovine F 18 is (1r, 3r)-1-amino-3[ 18F]fluorocyclobutane-1-carboxylic acid. The molecular weight is 132.1 and the structural formula is:
Axumin is a sterile, non-pyrogenic, clear, colorless, hyperosmolal (approximately 500 mOsm/kg to 540 mOsm/kg) injection for intravenous use. Each milliliter contains up to 2 micrograms of fluciclovine, 335 MBq to 8,200 MBq (9 mCi to 221 mCi) fluciclovine F 18 at calibration time and date, and 20 mg trisodium citrate in water for injection. The solution also contains hydrochloric acid, sodium hydroxide and has a pH between 4 and 6.
Fluorine 18 (F 18) is a cyclotron produced radionuclide that decays by positron emission (ß+ decay, 96.7%) and orbital electron capture (3.3%) to stable oxygen 18 with a physical half-life of 109.7 minutes. The positron can undergo annihilation with an electron to produce two gamma rays; the energy of each gamma ray is 511 keV ( Table 2).
Energy (keV) | Abundance (%) | |
Positron | 249.8 | 96.7 |
Gamma | 511.0 | 193.5 |
The point source air-kerma coefficient for F 18 is 3.75 x 10 -17Gy m 2/(Bq s). The first half-value thickness of lead (Pb) for F 18 gamma rays is approximately 6 mm. The relative reduction of radiation emitted by F 18 that results from various thicknesses of lead shielding is shown in Table 3. The use of 8 cm of Pb will decrease the radiation transmission (i.e., exposure) by a factor of about 10,000.
Shield Thickness cm of Lead (Pb) | Coefficient of Attenuation |
0.6 | 0.5 |
2 | 0.1 |
4 | 0.01 |
6 | 0.001 |
8 | 0.0001 |
Fluciclovine F 18 is a synthetic amino acid transported across mammalian cell membranes by amino acid transporters, such as LAT-1 and ASCT2, which are upregulated in prostate cancer cells. Fluciclovine F 18 is taken up to a greater extent in prostate cancer cells compared with surrounding normal tissues.
Following intravenous administration, the tumor-to-normal tissue contrast is highest between 4 and 10 minutes after injection, with a 61% reduction in mean tumor uptake at 90 minutes after injection.
Carcinogenesis
No long term studies in animals have been performed to evaluate the carcinogenic potential of fluciclovine.
Mutagenesis
Fluciclovine was not mutagenic in vitroin reverse mutation assay in bacterial cells and in chromosome aberration test in cultured mammalian cells, and was negative in an in vivoclastogenicity assay in rats after intravenous injection of doses up to 43 mcg/kg. However, fluciclovine F 18 has the potential to be mutagenic because of the F 18 radioisotope.
The safety and efficacy of Axumin were evaluated in two studies (Study 1 and Study 2) in men with suspected recurrence of prostate cancer based on rising PSA levels following radical prostatectomy and/or radiotherapy.
Study 1 evaluated 105 Axumin scans in comparison to histopathology obtained by biopsy of the prostate bed and biopsies of lesions suspicious by imaging. PET/CT imaging generally included the abdomen and pelvic regions. The Axumin images were originally read by on-site readers. The images were subsequently read by three blinded independent readers. Table 4shows the performance of Axumin in the detection of recurrence in each patient scan and, specifically, within the prostatic bed and extra-prostatic regions, respectively. The results of the independent read were generally consistent with one another and confirmed the results of the on-site reads.
N = number of patient scans evaluated |
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Reader 1 | Reader 2 | Reader 3 | |
Patient | N = 104 | N = 105 | N = 99 |
True Positive | 75 | 72 | 63 |
False Positive | 24 | 23 | 13 |
True Negative | 5 | 7 | 15 |
False Negative | 0 | 3 | 8 |
Prostate Bed | N = 98 | N = 97 | N = 96 |
True Positive | 58 | 56 | 47 |
False Positive | 29 | 26 | 15 |
True Negative | 10 | 12 | 24 |
False Negative | 1 | 3 | 10 |
Extraprostatic | N = 28 | N = 28 | N = 25 |
True Positive | 25 | 26 | 22 |
False Positive | 2 | 2 | 2 |
True Negative | 0 | 0 | 0 |
False Negative | 1 | 0 | 1 |
The detection rate of Axumin seems to be affected by PSA levels [see Warnings and Precautions ( 5.1)] . In general, patients with negative scans had lower PSA values than those with positive scans. The detection rate (number with positive scans/total scanned) for patients with a PSA value of less than or equal to 1.78 ng/mL (1st PSA quartile) was 15/25, of which 11 were histologically confirmed as positive. In the remaining three PSA quartiles, the detection rate was 71/74, of which 58 were histologically confirmed. Among the 25 patients in the first PSA quartile, there were 4 false positive scans and 1 false negative scan. For the 74 patients with PSA levels greater than1.78 ng/mL, there were 13 false positive scans and no false negative scans.
Study 2 evaluated the concordance between 96 Axumin and C11 choline scans in patients with median PSA value of 1.44 ng/mL (interquartile range = 0.78 ng/mL to 2.8 ng/mL). The C 11 choline scans were read by on-site readers. The Axumin scans were read by the same three blinded independent readers used for Study 1. The agreement values between the Axumin and C11 choline reads were 61%, 67% and 77%, respectively.
Axumin is supplied as a clear, colorless injection in a 30 mL or 50 mL multiple-dose glass vial containing approximately 26 mL solution of 335 MBq/mL to 8,200 MBq/mL (9 mCi/mL to 221 mCi/mL) fluciclovine F 18 at calibration time and date.
30 mL sterile multiple-dose vial: NDC 69932-001-30
50 mL sterile multiple-dose vial: NDC 69932-001-50
Store Axumin at controlled room temperature (USP) 20°C to 25°C (68°F to 77°F). Axumin does not contain a preservative. Store Axumin within the original container in radiation shielding. Do not use Axumin more than 10 hours after end of synthesis and dispose of in accordance with institutional guidelines.
This preparation is approved for use by persons under license by the Nuclear Regulatory Commission or the relevant regulatory authority of an Agreement State.
Marketed by Blue Earth Diagnostics Ltd. Oxford, UK OX4 4GA
Axumin
®is a registered trademark of Blue Earth Diagnostics Ltd.
© 2022 Blue Earth Diagnostics Ltd – all rights reserved.
Principal Display Panel - 30 mL Multiple-Dose Vial Label
Sterile
Axumin™
Non-pyrogenic
335 MBq/mL to 8,200 MBq/mL (9 mCi/mL to
221 mCi/mL) at End of Synthesis (EOS)
Diagnostic - For Intravenous Use Only
Expires 10 hours after EOS
Batch #: ________________________________
EOS Date: __________ EOS Time: __________
Activity @ EOS: ___________________ mCi
Concentration: ___________________ mCi/mL
Volume: ___________________ mL
Exp. Date: __________ Exp. Time: __________
AXUMIN
fluciclovine f-18 injection, solution |
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