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赖氨酸和精氨酸联合使用对放射性标记奥曲肽肾摄取的安全有效抑制作用。

Safe and effective inhibition of renal uptake of radiolabelled octreotide by a combination of lysine and arginine.

作者信息

Rolleman Edgar J, Valkema Roelf, de Jong Marion, Kooij Peter P M, Krenning Eric P

机构信息

Department of Nuclear Medicine, Erasmus Medical Centre, Dr. Molewaterplein 40, 3015 GD Rotterdam, The Netherlands.

出版信息

Eur J Nucl Med Mol Imaging. 2003 Jan;30(1):9-15. doi: 10.1007/s00259-002-0982-3. Epub 2002 Oct 29.

Abstract

As scintigraphy with [(111)In-DTPA(0)]octreotide has become a standard technique in analysing somatostatin receptor-receptor positive lesions such as neuroendocrine tumours, a logical next step is peptide receptor radionuclide therapy (PRRT). Initial studies on PRRT were performed with high doses of [(111)In-DTPA(0)]octreotide, and recently other radionuclides coupled to other somatostatin analogues have been used for this purpose. However, the dose delivered to the kidney is a major dose-limiting factor. Amino acid solutions have previously been used to reduce renal uptake of radioactivity, but these solutions have some disadvantages, i.e. their hyperosmolarity and their propensity to cause vomiting and metabolic changes. In this study we tested various amino acid solutions in patients receiving [(111)In-DTPA(0)]octreotide PRRT in order to assess their safety and their capacity to inhibit the renal uptake of radioactivity. Patients served as their own non-infused control. Renal radioactivity at 24 h following the injection of [(111)In-DTPA(0)]octreotide was inhibited by (1) a commercially available amino acid solution (AA) (21%+/-14%, P<0.02), (2) by 25 g (17%+/-9%, P<0.04), 50 g (15%+/-13%, P<0.04) or 75 g of lysine (44%+/-11%, P<0.001) and (3) by a combination of 25 g of lysine plus 25 g of arginine (LysArg) (33%+/-23%, P<0.01). Fluid infusion alone (500, 1,000 or 2,000 ml of saline/glucose) did not change renal uptake of radioactivity. In patients studied with 75 g of lysine (Lys75) and LysArg, serum potassium levels rose significantly. Maximal potassium levels were within the toxic range (6.3, 6.7 and 6.8 mmol/l) in three out of six patients infused with Lys75, whereas with LysArg the highest concentration measured was 6.0 mmol/l. Electrocardiographic analysis did not reveal significant changes in any of the patients. Vomiting occurred in 50% of patients infused with AA, but in only 6% of patients receiving no amino acid infusion (controls) and 9% of patients receiving LysArg. We conclude that co-infusion of Lys75 or LysArg results in a significant inhibition of renal radioactivity in PRRT, allowing higher treatment doses and thus resulting in higher tumour radiation doses. Because Lys75 produced serious hyperkalaemia, it is not suitable for clinical use. LysArg, however, is effective in offering renal protection in PRRT and is safe.

摘要

由于使用[(111)In - DTPA(0)]奥曲肽的闪烁扫描已成为分析生长抑素受体阳性病变(如神经内分泌肿瘤)的标准技术,接下来合理的一步是进行肽受体放射性核素治疗(PRRT)。最初关于PRRT的研究使用高剂量的[(111)In - DTPA(0)]奥曲肽,最近其他与其他生长抑素类似物偶联的放射性核素也被用于此目的。然而,输送到肾脏的剂量是一个主要的剂量限制因素。氨基酸溶液此前已被用于减少肾脏对放射性的摄取,但这些溶液有一些缺点,即它们的高渗性以及导致呕吐和代谢变化的倾向。在本研究中,我们在接受[(111)In - DTPA(0)]奥曲肽PRRT的患者中测试了各种氨基酸溶液,以评估其安全性及其抑制肾脏摄取放射性的能力。患者自身作为未输注的对照。注射[(111)In - DTPA(0)]奥曲肽后24小时的肾脏放射性受到以下因素抑制:(1)一种市售氨基酸溶液(AA)(21%±14%,P<0.02);(2)25克(17%±9%,P<0.04)、50克(15%±13%,P<0.04)或75克赖氨酸(44%±11%,P<0.001);(3)25克赖氨酸加25克精氨酸的组合(LysArg)(33%±23%,P<0.01)。单独输液(500、1000或2000毫升生理盐水/葡萄糖)并未改变肾脏对放射性的摄取。在使用75克赖氨酸(Lys75)和LysArg进行研究的患者中,血清钾水平显著升高。在输注Lys75的6名患者中有3名的最大钾水平处于中毒范围(6.3、6.7和6.8毫摩尔/升),而使用LysArg时测得的最高浓度为6.0毫摩尔/升。心电图分析未发现任何患者有显著变化。输注AA的患者中有50%发生呕吐,但未输注氨基酸的患者(对照组)中只有6%,接受LysArg的患者中有9%发生呕吐。我们得出结论,在PRRT中共同输注Lys75或LysArg可显著抑制肾脏放射性,允许使用更高的治疗剂量,从而导致更高的肿瘤辐射剂量。由于Lys75会导致严重的高钾血症,不适合临床使用。然而,LysArg在PRRT中能有效提供肾脏保护且安全。

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