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Development of New Capability for 211At Production

This project focuses on producing 211At for cancer therapy using innovative methods and accelerator technology. Leveraging the ATLAS facility for efficient production and distribution of this important radionuclide.

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Development of New Capability for 211At Production

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  1. The development of a new production capability for 211At Jerry Nolen, John Greene, Martin Alcorta, Bradley Micklich, Shaofei Zhu, Chithra Nair, and Irshad Ahmad, Physics Division Samuel Baker, Environment, Safety, & Quality Assurance Division Argonne National Laboratory Chin-Tu Chen, Sean S. H. Cheng, Leuwei Lo, and Patrick Michael, Department of Radiology Anhui Wu, Muriel Lainé, and Geoffrey Green, the Ben May Department for Cancer Research University of Chicago Michael Zalutsky, Duke University and University of Chicago This work was supported by the U.S. Department of Energy, Office of Nuclear Physics, under Contract No. DE-AC02-06CH11357. Health physics support: Fred Monette, Gordon Johnson, and Angel Garcia The 8th International Symposium on Targeted Alpha Therapy

  2. US Nuclear Science Advisory Committee Isotopes Panel Accelerator-Based Production of Medical Isotopes

  3. First recommendation of the NSAC-I panel Accelerator-Based Production of Medical Isotopes

  4. Addressing the shortage identified by the NSAC-I panel: expanding accelerator-based production of alpha-emitting isotopes • Case 1: production of 225Ac/213Bi and 211Rn/211At generators by proton spallation of thorium • Proposed by Argonne and ICGomes, Inc. • Large yield predicted for protons above 100 MeV • DOE funded for validation of 225Ac yields • Collaboration of Argonne, FermiLab, ICGomes, Inc., and NorthStar Medical Isotopes • Production test with FermiLab 8-GeV beam successfully completed in 2011 • Separation and purification chemistry was carried out at Argonne Chemistry Division • Case 2: production of 211At at low energies with alpha or lithium beams • Direct production of 211At (7-hour half-life) via the 209Bi(alpha,2n) reaction at alpha beam energy below 30 MeV to avoid 210At/210Po impurity • Production of 211At via 211Rn generator (14-hour half-life) via the 209Bi(7Li,5n) reaction • High power liquid-metal cooled target concept developed to enable extrapolation to high beam power • Subject of proposed DOE/ONP R&D at ANL/PHY/ATLAS Accelerator-Based Production of Medical Isotopes

  5. The development of a new production capability for 211At Abstract Critically needed radionuclides for cancer therapy include the alpha-emitter 211At and potentially therapeutically useful Auger-electron emitters. The ATLAS (Argonne Tandem Linac Accelerator System) superconducting linac at Argonne National Laboratory should be suitable for the production of these radionuclides. Our work is initially focusing on demonstrating production capabilities for 211At (7.2 h half-life) using the 209Bi(7Li,5n)211Rn or the 209Bi(6Li,4n)211Rn reaction. Cross sections for these reactions peak in the range of several hundred mb [1] making production of 10’s of mCi per batch feasible using only a very small percentage of the accelerator beam time. Presently, R&D with 211At is primarily at 3 facilities in the U.S. using the 209Bi(α,2n)211At reaction at in-house cyclotrons. R&D nation-wide with 211At is limited due to its short half-life. By using one of the lithium induced reactions, the 211At daughter is extracted from the parent 211Rn, which has a half-life of 14 h, significantly extending the time-frame for effective distribution and use of this important radionuclide. The impact of the half-life difference is illustrated in the figure below. ATLAS is an appropriate and flexible accelerator for the production of medical isotopes because it can provide beams of any ion including protons, helium, lithium, and heavier ions with energies adjustable over a wide range. An upgrade of the accelerator and the shielding is in progress. Following the completion of this work in the fall of 2013, currents of ion beams up to 10 particle microamps or more will be available. To fully implement isotope production capability using these more intense beams, a new irradiation cave has been proposed. These combined upgrades will enable yields of 100 mCi of 211Rn/211At using ~10 hours of beam time per batch. 1. Meyer GJ, Lambrecht RM, Excitation function for the 209Bi(7Li, 5n)211Rn nuclear reaction, Inter. J. of App. Rad. and Isotopes, 31(1980)351-355. Accelerator-Based Production of Medical Isotopes

  6. Excitation function for production of 211Rn precursor of 211At Accelerator-Based Production of Medical Isotopes

  7. The proposed development enables overnight delivery of 211At to any facility in the U.S. Accelerator-Based Production of Medical Isotopes

  8. Alpha vs. lithium advantages/disadvantages • Alpha  Cross section gives larger initial activity • Target must be dissolved each run • Dry distillation or wet extraction • Lithium  14 hour half-life > useful yield 1-3 days after production  Continuous extraction of 211Rn from the target • Simple physical extraction of 211At from the “generator” • R&D on lithium method in collaboration with Michael Zalutsky (Duke & Chicago) with interested users at Univ. Chicago Comprehensive Cancer Center Accelerator-Based Production of Medical Isotopes

  9. Location of proposed production cave in area 2 Accelerator-Based Production of Medical Isotopes

  10. Radiation handling at ATLAS Glove box and hood at ATLAS Accelerator-Based Production of Medical Isotopes

  11. Existing beam lines and apparatus at ATLAS Scattering chamber at ATLAS Accelerator-Based Production of Medical Isotopes

  12. Beamline and target assembly Health physicist, Post-doc, Undergraduate Target/ helium plumbing/ heater assembly Havar window 32 mg/cm2 Bi on Ni Accelerator-Based Production of Medical Isotopes

  13. Carbon trap and corn-oil bubblers Accelerator-Based Production of Medical Isotopes

  14. Activated carbon trap Accelerator-Based Production of Medical Isotopes

  15. Counting 211Rn trapped in charcoal (left)Counting 211At extracted from charcoal (right) Accelerator-Based Production of Medical Isotopes

  16. Target assembly, 211Rn trap, 211At elution

  17. X-ray Spectra of elution from charcoal x-rays from 211At electron capture, no 207Po, no 211Rn Accelerator-Based Production of Medical Isotopes

  18. Summary • Clinically useful quantities of the alpha emitter 211At can be produced with low energy light ions at the upgraded ANL/PHY ATLAS facility using small fraction of the annual beam time • The production via the 211Rn/211At generator approach can greatly extend the national availability of this isotope by effectively doubling its life-time • R&D of this alternative method began recently with a test run at ATLAS • Next step to use RGA to measure continuous release of Xe from hot, solid Bi Accelerator-Based Production of Medical Isotopes

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