Multiple Production Methods Underway to Provide Actinium-225 | NIDC: National Isotope Development Center

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Ac-225 in vial — Actinium-225 in a vial.

Discovered in 1947 by a team at Argonne National Laboratory and an independent Canadian research team, actinium-225 (Ac-225) undergoes alpha decay to francium-221 with a half-life of 10 days. For this reason, the isotope is being evaluated as an ideal candidate for use in medical applications. Alpha-emitting isotopes show great promise for cancer treatment because of their short path length and high energy transfer of radiation. Typically, the range is only that of a few cell diameters, making these isotopes highly effective at destroying cancer cells and leaving healthy cells untouched. Many radiolabeled products that incorporate Ac-225 are currently being used in numerous clinical trials for the treatment of cancers including prostate cancer, myeloid leukemia, and breast cancer.

The U.S. Department of Energy Isotope Program (DOE IP) identified Ac-225 as a critical isotope because of its high demand and limited availability. Over the last 10+ years, the DOE IP has provided funding and facilities to aid in the research and development of new methods for creating the isotope. Also of considerable interest in the medical community is the daughter isotope of Ac-225, bismuth-213 (Bi-213), which has applications as the radioactive component in cancer treatment options for leukemia, lymphomas, and micrometastatic carcinomas.

Production Methods for Ac-225

Presently, the primary source of Ac-225 comes from thorium-229 (Th-229) decay. Stores of Th-229 were considered a waste product, leftover from nuclear programs in the 1940s and 1950s. For many years, Th-229 was stored in a secure facility—until the discovery that Ac-225 and its decay daughter, Bi-213, what is a smart quote were of great medical interest. Scientists at Oak Ridge National Laboratory (ORNL) began "milking" the stores of Th-229—a process that involves separating Ac-225 from the other isotopes that decay from thorium. The process is repeated every month, with each batch yielding millicurie quantities of Ac-225.

The demand for Ac-225 is growing daily with researchers, physicians, and patients around the world waiting for shipments of the radionuclide, which is then radiolabeled to yield individual patient doses. To address global demand and assist in providing this rare and critical isotope, the DOE IP organized facility usage and funding to research multiple routes for producing Ac-225. One of these methods, accelerator-produced actinium-225, is being investigated by three national laboratories and was coined the Ac-225 Tri-Lab Effort.

Ac-225 Tri-Lab Effort

The Brookhaven Linac Isotope Producer (BLIP)

The Ac-225 Tri-Lab Effort was established in 2015 by the DOE IP and researchers at Brookhaven, Los Alamos, and Oak Ridge National Laboratories to research and develop new production routes for Ac-225. Using accelerator beam facilities at Brookhaven and Los Alamos, thorium-232 targets are fabricated at the labs and placed into an accelerator. After bombardment, the targets are removed and shipped to ORNL for chemical processing, and finally, the purified product is shipped to customers. The goal of the Ac-225 Tri-Lab Effort is to leverage DOE IP facilities, capabilities, and expertise to fill the void in supply for the medical and research Ac-225 markets.

Since its formation, the Tri-Lab Effort has distributed more than 275 mCi of accelerator-produced Ac-225 to evaluators. In 2019, the group announced routine production and product availability for purchase by end-users. Plans for the effort include producing greater quantities of the isotope—from the current 50–100 mCi per batch to 100–1,000 mCi per batch over the next 4 years. Renovations to existing processing facilities at Brookhaven National Laboratory and construction of a new building at Los Alamos National Laboratory are underway, allowing the DOE IP and Tri-Lab Effort to accomplish these goals.

FDA accepts Drug Master File for actinium-225 nitrate (accelerator-produced)

In January 2020, the U.S. Food and Drug Administration (FDA) accepted a Type II Drug Master File (DMF) submission for actinium-225 nitrate (accelerator-produced) submitted by ORNL.

Visit our Ac-225 DMF Announcement

A milestone for the Tri-Lab Effort, a DMF is a confidential, detailed document submitted to the FDA with information about facilities, processes, or articles used in the manufacturing, processing, packaging and storing of human drug products. An active DMF enables clinical investigators and pharmaceutical companies to reference the filing in their regulatory submissions.

Click Here to Request a Quote for Actinium-225

For more information on Ac-225 and the Tri-Lab Effort, click the links below.

2020 Ac-225 User Meeting Recording

Ac-225 User Meeting Recording

Watch the Actinium-225 User Meeting Video

2020 Ac-225 User Meeting Presentations

Kate Dadachova with the University of Saskatchewan — Ac-225 User Meeting Introduction by Kate Dadachova, University of Saskatchewan

Ac-225 Users Meeting_Cutler — *Production Effort to Provide Accelerator-Produced Ac-225 for Radiotherapy* by Dr. Cathy Culter, Brookhaven National Laboratory

Ac-225 Users Meeting_Ravindra — Ac-225 Radiopharmaceuticals FDA Perspective - Chemistry,
Manufacturing, and Controls
by Dr. Ravindra Kasliwal, U.S. FDA

Ac-225 Users Meeting_Dimmick — *NRC Perspectives on Emerging Radionuclides* by Lisa Dimmick, U.S. NRC

Ac-225 Users Meeting_Sanders — *Radiolabeling Comparison of Accelerator Versus Generator Produced Ac-225* by Dr. Vanessa Sander, Brookhaven National Laboratory

Ac-225 Users Meeting_Allen — *Ac-225 and Bi-213: Two Important Alpha-Emitters for the Future of Therapeutics* by Dr. Kevin Allen, University of Saskatchewan

Ac-225 Users Meeting_Jurcic — *Targeted Alpha-Particle Therapy for Acute Myeloid Leukemia* by Dr. Joseph Jurcic, Columbia University

Brochures

Tri-Lab brochure — Actinium-225 Tri-Lab Brochure

Patents

Lime Patent Icon — U.S. Patent: Separation of Actinium and Radium Isotopes from a Proton-Irradiated Thorium Matrix | Patent # 9,951,399 | Apr. 24, 2018

Teal Patent Icon — Actinium-225 Compositions of Matter and Methods of Their Use | Patent # 9,555,140 | Jan. 31, 2017

Dark Gray patent icon — Actinium-225 Compositions of Matter and Methods of Their Use | Patent # 10,391,186 | Aug. 27, 2019

Posters

Ac-225 Tri-Lab Production Effort 2019 Update

Ac-225 Radiolabeling Poster_Ludwig — Radiolabeling of DOTA-conjugated Lintuzumab with Ac-225

Publications – Ac-225 Dosimetry

Dosimetric Impact of Ac-227 in Accelerator-produced Ac-225

In vivo Evaluation of Free and Chelated Accelerator-produced Ac-225 - Radiation Dosimetry and Toxicity Results

Publications – Production of Ac-225

Proton Induced Cross Sections Relevant to Production of Ac-225 and Ra-223 in Natural Thorium Targets Below 200 MeV	Cross Sections From Proton Irradiation of Thorium at 800 MeV	Production of Medical Isotopes From a Thorium Target Irradiated By Light Charged Particles Up to 70 MeV	Optimization of Cation Exchange for the Separation of Actinium-225 From Radioactive Thorium, Radium-223, and Other Metals
Large-Scale Accelerator Production of Ac-225: Effective Cross Sections for 78–192 MeV Protons Incident on Th-232 Targets	Defining Process Times for Accelerator Produced Actinium-225 and Other Isotopes from Proton Irradiated Thorium	Radiometric Evaluation of Diglycolamide Resins for the Chromatographic Separation of Actinium From Fission Product Lanthanides	The Application of Poorly Crystalline Silicotitanate in Production of Ac-225

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