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在高比活度下用90Y、111In和177Lu对DOTA肽进行放射性标记的条件优化。

Optimising conditions for radiolabelling of DOTA-peptides with 90Y, 111In and 177Lu at high specific activities.

作者信息

Breeman Wouter A P, De Jong Marion, Visser Theo J, Erion Jack L, Krenning Eric P

机构信息

Department of Nuclear Medicine, Erasmus MC Rotterdam, The Netherlands.

出版信息

Eur J Nucl Med Mol Imaging. 2003 Jun;30(6):917-20. doi: 10.1007/s00259-003-1142-0. Epub 2003 Apr 4.

Abstract

DOTA-conjugated peptides, such as [DOTA(0),Tyr(3)]octreotide (DOTATOC) and [DOTA(0),Tyr(3)]octreotate (DOTA-tate), can be labelled with radionuclides such as (90)Y, (111)In and (177)Lu. These radiolabelled somatostatin analogues are used for peptide receptor radionuclide therapy (PRRT). Radioligands for PRRT require high specific activities. However, although these radionuclides are produced without addition of carrier, contaminants are introduced during production and as decay products. In this study, parameters influencing the kinetics of labelling of DOTA-peptides were investigated and conditions were optimised to obtain the highest achievable specific activity. The effects of contaminants were systematically investigated, concentration dependently, in a test model mimicking conditions for labelling with minimal molar excess of DOTA-peptides over radionuclide. Kinetics of labelling of DOTA-peptides were optimal at pH 4-4.5; pH <4 strongly slowed down the kinetics. Above pH 5, reaction kinetics varied owing to the formation of radionuclide hydroxides. Labelling with (90)Y and (177)Lu was completed after 20 min at 80 degrees C, while labelling with (111)In was completed after 30 min at 100 degrees C. The effects of contaminants were systematically categorised, e.g. Cd(2+) is the target and decay product of (111)In, and it was found to be a strong competitor with (111)In for incorporation in DOTA. In contrast, Zr(4+) and Hf(4+), decay products of (90)Y and (177)Lu, respectively, did not interfere with the incorporation of these radionuclides. The following conclusions are drawn: (a) DOTA-peptides can be radiolabelled at high specific activity; (b) reaction kinetics differ for each radionuclide; and (c) reactions can be hampered by contaminants, such as target material and decay products.

摘要

与DOTA共轭的肽,如[DOTA(0),Tyr(3)]奥曲肽(DOTATOC)和[DOTA(0),Tyr(3)]奥曲肽(DOTA-泰特),可使用诸如(90)Y、(111)In和(177)Lu等放射性核素进行标记。这些放射性标记的生长抑素类似物用于肽受体放射性核素治疗(PRRT)。PRRT的放射性配体需要高比活度。然而,尽管这些放射性核素在生产过程中未添加载体,但在生产过程中以及作为衰变产物会引入污染物。在本研究中,研究了影响DOTA肽标记动力学的参数,并优化了条件以获得最高可实现的比活度。在模拟DOTA肽相对于放射性核素摩尔过量最小的标记条件的测试模型中,系统地研究了污染物浓度依赖性的影响。DOTA肽的标记动力学在pH 4 - 4.5时最佳;pH <4会强烈减慢动力学。pH高于5时,由于放射性核素氢氧化物的形成,反应动力学有所不同。用(90)Y和(177)Lu标记在80℃下20分钟后完成,而用(111)In标记在100℃下30分钟后完成。污染物的影响被系统地分类,例如Cd(2+)是(111)In的靶标和衰变产物,并且发现它是(111)In掺入DOTA的强竞争者。相反,分别是(90)Y和(177)Lu衰变产物的Zr(4+)和Hf(4+)不会干扰这些放射性核素的掺入。得出以下结论:(a)DOTA肽可以高比活度进行放射性标记;(b)每种放射性核素的反应动力学不同;(c)反应可能会受到污染物(如靶物质和衰变产物)的阻碍。

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