Theranostic Terbium Radioisotopes: Challenges in Production for Clinical Application

核素 放射性核素 放射化学 同位素 核物理学 回旋加速器 中子 化学 物理 离子 等离子体 有机化学
作者
Nabanita Naskar,Susanta Lahiri
出处
期刊:Frontiers in Medicine [Frontiers Media]
卷期号:8 被引量:55
标识
DOI:10.3389/fmed.2021.675014
摘要

Currently, research on terbium has gained a momentum owing to its four short-lived radioisotopes, 149 Tb, 152 Tb, 155 Tb, and 161 Tb, all of which can be considered in one or another field of nuclear medicine. The members of this emerging quadruplet family have appealing nuclear characteristics and have the potential to do justice to the proposed theory of theranostics nuclear medicine, which amalgamates therapeutic and diagnostic radioisotopes together. The main challenge for in vivo use of these radioisotopes is to produce them in sufficient quantity. This review discusses that, at present, neither light charged particle nor the heavy ion (HI) activation are suitable for large-scale production of neutron deficient terbium nuclides. Three technological factors like (i) enrichment of stable isotopes to a considerable level, (ii) non-availability of higher energies in commercial cyclotrons, and (iii) non-availability of the isotope separation technique coupled with commercial accelerators limit the large scale production of terbium radionuclides by light charged particle activation. If in future, the technology can overcome these hurdles, then the light charged particle activation of enriched targets would produce a high amount of useful terbium radionuclides. On the other hand, to date, the spallation reaction coupled with an online isotope separator has been found suitable for such a requirement, which has been adopted by the CERN MEDICIS programme. The therapeutic 161 Tb radionuclide can be produced in a reactor by neutron bombardment on enriched 160 Gd target to produce 161 Gd which subsequently decays to 161 Tb. The radiochemical separation is mandatory even if the ISOL technique is used to obtain high radioisotopic purity of the desired radioisotope.
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