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用于α粒子介导放射免疫治疗的锕-225的制备。

Production of actinium-225 for alpha particle mediated radioimmunotherapy.

作者信息

Boll Rose A, Malkemus Dairin, Mirzadeh Saed

机构信息

Nuclear Science and Technology Division, Oak Ridge National Laboratory, Oak Ridge, TN 37831-6229, USA.

出版信息

Appl Radiat Isot. 2005 May;62(5):667-79. doi: 10.1016/j.apradiso.2004.12.003. Epub 2005 Jan 28.

Abstract

The initial clinical trials for treatment of acute myeloid leukemia have demonstrated the effectiveness of the alpha emitter (213)Bi in killing cancer cells. Bismuth-213 is obtained from a radionuclide generator system from decay of 10-days (225)Ac parent. Recent pre-clinical studies have also shown the potential application of both (213)Bi, and the (225)Ac parent radionuclide in a variety of cancer systems and targeted radiotherapy. This paper describes our five years of experience in production of (225)Ac in partial support of the on-going clinical trials. A four-step chemical process, consisting of both anion and cation exchange chromatography, is utilized for routine separation of carrier-free (225)Ac from a mixture of (228)Th, (229)Th and (232)Th. The separation of Ra and Ac from Th is achieved using the marcoporous anion exchange resin MP1 in 8M HNO(3) media. Two sequential MP1/NO(3) columns provide a separation factor of approximately 10(6) for Ra and Ac from Th. The separation of Ac from Ra is accomplished on a low cross-linking cation exchange resin AG50-X4 using 1.2M HNO(3) as eluant. Two sequential AG50/NO(3) columns provide a separation factor of approximately 10(2) for Ac from Ra. A 60-day processing schedule has been adopted in order to reduce the processing cost and to provide the highest levels of (225)Ac possible. Over an 8-week campaign, a total of approximately 100 mCi of (225)Ac (approximately 80% of the theoretical yield) is shipped in 5-6 batches, with the first batch typically consisting of approximately 50 mCi. After the initial separation and purification of Ac, the Ra pool is re-processed on a bi-weekly schedule or as needed to provide smaller batches of (225)Ac. The averaged radioisotopic purity of the (225)Ac was 99.6 +/- 0.7% with a (225)Ra content of < or =0.6%, and an average (229)Th content of (4(-4)(+5)) x 10(-5)%.

摘要

治疗急性髓系白血病的初步临床试验已证明α发射体(213)Bi在杀死癌细胞方面的有效性。铋 - 213是从10天(225)Ac母体衰变的放射性核素发生器系统中获得的。最近的临床前研究也表明(213)Bi和(225)Ac母体放射性核素在各种癌症系统和靶向放射治疗中的潜在应用。本文描述了我们在生产(225)Ac方面五年的经验,以部分支持正在进行的临床试验。一个由阴离子和阳离子交换色谱组成的四步化学过程,用于从(228)Th、(229)Th和(232)Th的混合物中常规分离无载体(225)Ac。在8M HNO₃介质中使用大孔阴离子交换树脂MP1实现从钍中分离镭和锕。两个连续的MP1/NO₃柱对镭和锕与钍的分离因子约为10⁶。使用1.2M HNO₃作为洗脱剂,在低交联阳离子交换树脂AG50 - X4上完成从镭中分离锕。两个连续的AG50/NO₃柱对锕与镭的分离因子约为10²。为了降低处理成本并提供尽可能高产量的(225)Ac,采用了60天的处理时间表。在为期8周的活动中,总共约100 mCi的(225)Ac(约为理论产量的80%)分5 - 6批运送,第一批通常约为50 mCi。锕初步分离和纯化后,镭库按双周时间表或根据需要重新处理,以提供较小批次的(225)Ac。(225)Ac的平均放射性同位素纯度为99.6±0.7%,(225)Ra含量≤0.6%,平均(229)Th含量为(4⁻⁴⁺⁵)×10⁻⁵%。

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