Targeted alpha therapy for cancer

Allen, Barry J.; Raja, Chand; Rizvi, Syed Monem; Li, Yong; Tsui, Wendy; Zhang, David; Song, Emma; Qu, Chang; Kearsley, John H.; Graham, Peter; Thompson, John F.

doi:10.1088/0031-9155/49/16/016

Cited by 60 publications

(42 citation statements)

References 24 publications

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“…The average [range] radiation absorbed dose delivered to the tumor SCRC margin was 2764 [155-35,000] Gy, reflecting in large part the fact that cavity volumes for these patients varied from 0.2 cm 3 to 37.2 cm. 3 As shown in Figure 2, median survival for GBM patients (n=14) and all patients (n=18) was 52 and 56.5 weeks, respectively. Particularly encouraging is the fact that 2 of these recurrent GBM patients survived for 150 and 151 weeks after 211 At-labeled mAb treatment, which is considerably better than that obtained with conventional treatments (25-30 weeks).…”

Section: Clinical Evaluation Of 211 At-labeled Chimeric 81c6 Mabmentioning

confidence: 88%

“…Targeting α-particle emitting radionuclides to cancer cells has emerged as a particularly promising approach to molecular radiotherapy based on accumulating evidence from preclinical studies, as summarized in several recent reviews [1][2][3]. Because the range of α-particles in tissue is only about 50-80 μm, equivalent to only a few cell diameters, at least on a conceptual level, they are well matched to the cellular specificity of molecularly specific targeting vehicles, and minimize irradiation of tumor-adjacent normal tissues.…”

Section: Introductionmentioning

confidence: 99%

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Targeted α-particle radiotherapy with 211At-labeled monoclonal antibodies

Zalutsky

Reardon

Pozzi

et al. 2007

Nuclear Medicine and Biology

111

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An attractive feature of targeted radionuclide therapy is the ability to select radionuclides and targeting vehicles with characteristics that are best suited for a particular clinical application. One combination that has been receiving increasing attention is the use of monoclonal antibodies specifically reactive to receptors and antigens that are expressed on tumor cells to selectively deliver the α-particle emitting radiohalogen 211 At to malignant cell populations. Promising results have been obtained in preclinical models with multiple 211 At-labeled mAbs; however, translation of concept to the clinic has been slow. Impediments to this process include limited radionuclide availability, the need for suitable radiochemistry methods operant at high activity levels, and the lack of data concerning toxicity of α-particle emitters in humans. Nonetheless, two clinical trials have been initiated to date with 211 At-labeled monoclonal antibodies and others are planned for the near future.

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Section: Clinical Evaluation Of 211 At-labeled Chimeric 81c6 Mabmentioning

confidence: 88%

Section: Introductionmentioning

confidence: 99%

Targeted α-particle radiotherapy with 211At-labeled monoclonal antibodies

Zalutsky

Reardon

Pozzi

et al. 2007

Nuclear Medicine and Biology

111

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“…Microdosimetry technique can measure the microscopic distribution of energy from different types of radiation. Using the Monte Carlo models for biological dosimetry, the location and form of radionuclides within cells can be used to estimate radiation dose distributions and effects (47).…”

Section: Microdosimetrymentioning

confidence: 99%

Targeted Alpha Therapy Trial in Bangladesh: Promise for Advanced MUC1 – Expressing Tumors

Nisa¹,

Quadir

Begum

et al. 2018

Bangladesh J. Nuclear Med.

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“…helium nuclei) are quite large, have high energies of several MeV, and are associated with high probability of inflicting irreparable and cytocidal DNA double-strand breaks. 29 Consequently, α-emitters are well suited for hematologic disease, micrometastatic disease, and tumor cells near the surface of cavities.…”

Section: Radiobiology and Dosimetrymentioning

confidence: 99%

Development of radioimmunotherapeutic and diagnostic antibodies: an inside-out view

Boswell

Brechbiel

2007

Nuclear Medicine and Biology

215

213

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Only a handful of radiolabeled antibodies (Abs) have gained FDA approval for use in clinical oncology, including four immunodiagnostic agents and two targeted radioimmunotherapeutic agents. Despite the advent of non-immunogenic Abs and availability of a diverse library of radionuclides, progress beyond early Phase II RIT studies in solid tumors has been marginal. Furthermore, 18 F-FDG continues to dominate the molecular imaging domain, underscored by a decade-long absence of any newly approved antibody-based imaging agents (none since 1996!). Why has the development of clinically successful Abs for RIT been limited to lymphoma? What obstacles must be overcome to allow the FDA-approval of immunoPET imaging agents? How can we address the unique challenges that have thus far prevented the introduction of Ab-based imaging agents and therapeutics for solid tumors? Many poor decisions have been made regarding radiolabeled Abs, but useful insight can be gained from these mistakes. The following review addresses physical, chemical, biological, clinical, regulatory, and financial limitations that impede the progress of this increasingly important class of drugs. OverviewThe following review illustrates key components of a successful radiolabeled diagnostic or therapeutic antibody (Ab) from the inside out -that is, starting from the unstable nucleus itself and moving outwards. For each sequential topic, relevant theory will be examined and related to the practical use of various radiolabeled Abs that have succeeded to varying degrees in the clinic. This approach will present each important aspect of a rather complex multidisplinary phenomenon in a logical, stepwise manner: I. The radionuclide itselfPhysical properties of the unstable nucleus II. The radionuclide's chemical surroundingsChemical attachment of the radiometal or radiohalogen III. The antibodyBiological issues of the radioimmunoconjugate † Portions of this article were highlighted during a presentation at the Workshop on Molecular Imaging: After Bench to Bedside: Impact on Clinical Outcome Feb. [23][24][25] 2007. *Correspondence to: Martin W. Brechbiel, Ph.D., Radioimmune & Inorganic Chemistry Section, Radiation Oncology Branch, NCI, NIH, Building 10, Room 1B40, 10 Center Drive, Bethesda, MD 20892-1088, Fax: (301) 402-1923, e-mail: martinwb@mail.nih.gov. Publisher's Disclaimer: This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final citable form. Please note that during the production process errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. NIH Public Access Author ManuscriptNucl Med Biol. Author manuscript; available in PMC 2008 October 1. Published in final edited form as:Nucl Med Biol. 2007 October ; 34(7): 757-778. NIH-PA Author ManuscriptNIH-PA...

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Targeted alpha therapy for cancer

Cited by 60 publications

References 24 publications

Targeted α-particle radiotherapy with 211At-labeled monoclonal antibodies

Targeted α-particle radiotherapy with 211At-labeled monoclonal antibodies

Targeted Alpha Therapy Trial in Bangladesh: Promise for Advanced MUC1 – Expressing Tumors

Development of radioimmunotherapeutic and diagnostic antibodies: an inside-out view

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