Detailed Chemistry Studies of 225Actinium Labeled Radiopharmaceuticals.

IF 1.5 4区 医学 Q3 PHARMACOLOGY & PHARMACY Current radiopharmaceuticals Pub Date : 2022-01-01 DOI:10.2174/1874471014666210528123936
Kurtulus Eryilmaz, Benan Kilbas
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引用次数: 1

Abstract

Background: The synthesis of 225Actinium derivatives was afforded by using PSMA- 617, DOTATATE peptides, and EDTMP ligand. Detailed experiments, quality control (QC), and stability studies were also well described. The radiolabelling reactions were performed in mild conditions with desirable radiochemical yields and high radiochemical purities.

Methods: PSMA-617, DOTATATE were radiolabelled with 225Actinium in 0.1 M HCl in the presence of ascorbate buffer solution and passed through the C-18 light cartridge for purification and the product was eluted by ethanol-water solution. EDTMP was also radiolabelled with 225Actinium without using any stabilizer and purification step. All products were well analyzed by R-TLC and R-HPLC. The stability of those compounds was also studied within the validity period of time.

Results: 225Ac-DOTATATE and 225Ac-PSMA-617 were obtained at the same condition. The radiochemical yield of 225Ac-DOTATATE was less than225Ac-PSMA 617. The stability experiments indicating decay daughters of 225Actinium appeared after T0 +1 h due to the recoil effect radiolysis. On the other hand, 225Ac-EDTMP was more stable than DOTA-peptide radiolabelled compounds. 225Ac-EDTMP was produced with more than 95% radiochemical yield and 99% radiochemical purity.

Conclusion: A detailed chemistry study was presented for the synthesis of 225Actinium derivatives in mild conditions with absolute radiochemical purities and high yields. The experimental results showed that 225Ac-EDTMP could be a suitable radiopharmaceutical alternative for bone metastases arising from primer tumors as a cocktail therapy.

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225锕标记放射性药物的详细化学研究。
背景:采用PSMA- 617、DOTATATE多肽和EDTMP配体合成了225Actinium衍生物。详细的实验,质量控制(QC)和稳定性研究也很好地描述。放射性标记反应在温和的条件下进行,具有理想的放射化学产率和高放射化学纯度。方法:PSMA-617、DOTATATE在抗坏血酸缓冲液存在下,用225Actinium在0.1 M HCl中放射性标记,通过C-18光盒纯化,用乙醇-水溶液洗脱。EDTMP也用225Actinium进行放射性标记,不使用任何稳定剂和纯化步骤。所有产品均经R-TLC和R-HPLC分析。并在有效期内对这些化合物的稳定性进行了研究。结果:在相同条件下获得225Ac-DOTATATE和225Ac-PSMA-617。225Ac-DOTATATE的放射化学产率小于225ac - psma 617。稳定性实验表明,225Actinium在T0 +1 h后由于反冲效应而出现衰变子。另一方面,225Ac-EDTMP比dota肽放射性标记的化合物更稳定。225Ac-EDTMP的放射化学产率大于95%,放射化学纯度大于99%。结论:在温和的条件下合成了具有绝对放射化学纯度和高收率的225Actinium衍生物。实验结果表明,225Ac-EDTMP作为鸡尾酒疗法可作为引物肿瘤骨转移的一种合适的放射性药物替代方案。
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来源期刊
Current radiopharmaceuticals
Current radiopharmaceuticals PHARMACOLOGY & PHARMACY-
CiteScore
3.20
自引率
4.30%
发文量
43
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