4.4 Article

Positive Progress in ImmunoPET-Not Just a Coincidence

期刊

CANCER BIOTHERAPY AND RADIOPHARMACEUTICALS
卷 25, 期 3, 页码 253-261

出版社

MARY ANN LIEBERT, INC
DOI: 10.1089/cbr.2010.0776

关键词

antibody; cancer; molecular imaging; positron emission tomography (PET); radionuclide

资金

  1. UCLA SPORE in Prostate Cancer (NIH) [CA 092131]
  2. UCLA Center for In Vivo Imaging in Cancer Biology (NIH) [CA 086306]
  3. Stanford Center for Nanotechnology Excellence (NIH) [CA 119367]
  4. Dr. Ursula Mandel Scholarship

向作者/读者索取更多资源

The identification of tumor tissue biomarkers has led to the production, validation, and Food and Drug Administration-approval of a number of antibody-based targeted therapeutics in the past two decades. As a result of the significant role that these immunotherapeutics play in the management of cancer, and the potential utility of complementary imaging agents, immunoPET imaging has generated considerable interest. This update discusses the important factors to consider when designing a PET (positron emission tomography) imaging agent from the molecular target to the biological targeting molecule and radionuclide combination and also reviews recent preclinical and clinical findings in the immunoPET field. Although there are a variety of radionuclides that are currently utilized in PET studies, this update focuses on four of the positron emitters commonly used in labeling proteins: iodine-124, zirconium-89, copper-64, and fluorine-18. Notable advances in the preclinical setting include the continued development of immunoPET probes to predict the biodistribution of related radioimmunotherapeutics, the success of nontraditional radionuclide and antibody fragment combinations, the broader use of zirconium-89, and the recent emergence of 18 F-labeled diabodies for same-day imaging. Antibody-based PET probes constitute a valuable class of molecular imaging agents, and the progress made preclinically should expedite the transition of these targeted diagnostics to clinical applications.

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