Alpha-peptide receptor radionuclide therapy using actinium-225 labeled somatostatin receptor agonists and antagonists

被引:23
|
作者
Shi, Mengqi [1 ,2 ]
Jakobsson, Vivianne [1 ,3 ]
Greifenstein, Lukas [4 ]
Khong, Pek-Lan [1 ,5 ]
Chen, Xiaoyuan [1 ,2 ,5 ,6 ,7 ,8 ]
Baum, Richard P. [4 ]
Zhang, Jingjing [1 ,2 ,5 ]
机构
[1] Natl Univ Singapore, Yong Loo Lin Sch Med, Dept Diagnost Radiol, Singapore, Singapore
[2] Natl Univ Singapore, NUS Ctr Nanomed, Yong Loo Lin Sch Med, Nanomed Translat Res Program, Singapore, Singapore
[3] Acad Precis Oncol, Int Ctr Precis Oncol ICPO, Wiesbaden, Germany
[4] CURANOSTICUM Wiesbaden Frankfurt, Ctr Adv Radiomol Precis Oncol, Wiesbaden, Germany
[5] Natl Univ Singapore, Clin Imaging Res Ctr, Ctr Translat Med, Yong Loo Lin Sch Med, Singapore, Singapore
[6] Natl Univ Singapore, Yong Loo Lin Sch Med, Dept Surg Chem & Biomol Engn, Singapore, Singapore
[7] Natl Univ Singapore, Coll Design & Engn, Singapore, Singapore
[8] ASTAR, Inst Mol & Cell Biol, Singapore, Singapore
关键词
actinium-225; neuroendocrine tumor; peptide receptor radionuclide therapy (PRRT); targeted alpha-particle therapy; SSTR; SSTR antagonist; METASTATIC NEUROENDOCRINE TUMOR; RESISTANT PROSTATE-CANCER; IN-VIVO; PARTICLE THERAPY; POSITIVE TUMORS; AC-225; EXPRESSION; PATIENT; PET; DOSIMETRY;
D O I
10.3389/fmed.2022.1034315
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Peptide receptor radionuclide therapy (PRRT) has over the last two decades emerged as a very promising approach to treat neuroendocrine tumors (NETs) with rapidly expanding clinical applications. By chelating a radiometal to a somatostatin receptor (SSTR) ligand, radiation can be delivered to cancer cells with high precision. Unlike conventional external beam radiotherapy, PRRT utilizes primarily beta or alpha radiation derived from nuclear decay, which causes damage to cancer cells in the immediate proximity by irreversible direct or indirect ionization of the cells' DNA, which induces apoptosis. In addition, to avoid damage to surrounding normal cells, PRRT privileges the use of radionuclides that have little penetrating and more energetic (and thus more ionizing) radiations. To date, the most frequently radioisotopes are beta(-) emitters, particularly Yttrium-90 (Y-90) and Lutetium-177 (Lu-177), labeled SSTR agonists. Current development of SSTR-targeting is triggering the shift from using SSTR agonists to antagonists for PRRT. Furthermore, targeted alpha-particle therapy (TAT), has attracted special attention for the treatment of tumors and offers an improved therapeutic option for patients resistant to conventional treatments or even beta-irradiation treatment. Due to its short range and high linear energy transfer (LET), alpha-particles significantly damage the targeted cancer cells while causing minimal cytotoxicity toward surrounding normal tissue. Actinium-225 (Ac-225) has been developed into potent targeting drug constructs including somatostatin-receptor-based radiopharmaceuticals and is in early clinical use against multiple neuroendocrine tumor types. In this article, we give a review of preclinical and clinical applications of Ac-225-PRRT in NETs, discuss the strengths and challenges of Ac-225 complexes being used in PRRT; and envision the prospect of Ac-225-PRRT as a future alternative in the treatment of NETs.
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页数:18
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