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用于硼中子俘获治疗的治疗剂对硼苯丙氨酸(BPA)的质子核磁共振测量

Proton nuclear magnetic resonance measurement of p-boronophenylalanine (BPA): a therapeutic agent for boron neutron capture therapy.

作者信息

Zuo C S, Prasad P V, Busse P, Tang L, Zamenhof R G

机构信息

Department of Radiology, Beth Israel Deaconess Medical Center and Harvard Medical School, Boston, Massachusetts 02215, USA.

出版信息

Med Phys. 1999 Jul;26(7):1230-6. doi: 10.1118/1.598617.

Abstract

Noninvasive in vivo quantitation of boron is necessary for obtaining pharmacokinetic data on candidate boronated delivery agents developed for boron neutron capture therapy (BNCT). Such data, in turn, would facilitate the optimization of the temporal sequence of boronated drug infusion and neutron irradiation. Current approaches to obtaining such pharmacokinetic data include: positron emission tomography employing F-18 labeled boronated delivery agents (e.g., p-boronophenylalanine), ex vivo neutron activation analysis of blood (and very occasionally tissue) samples, and nuclear magnetic resonance (NMR) techniques. In general, NMR approaches have been hindered by very poor signal to noise achieved due to the large quadrupole moments of B-10 and B-11 and (in the case of B-10) very low gyromagnetic ratio, combined with low physiological concentrations of these isotopes under clinical conditions. This preliminary study examines the feasibility of proton NMR spectroscopy for such applications. We have utilized proton NMR spectroscopy to investigate the detectability of p-boronophenylalanine fructose (BPA-f) at typical physiological concentrations encountered in BNCT. BPA-f is one of the two boron delivery agents currently undergoing clinical phase-I/II trials in the U.S., Japan, and Europe. This study includes high-resolution 1H spectroscopic characterization of BPA-f to identify useful spectral features for purposes of detection and quantification. The study examines potential interferences, demonstrates a linear NMR signal response with concentration, and presents BPA NMR spectra in ex vivo blood samples and in vivo brain tissues.

摘要

对于为硼中子俘获疗法(BNCT)开发的候选硼化递送剂获取药代动力学数据而言,硼的无创体内定量分析是必要的。反过来,这些数据将有助于优化硼化药物输注和中子照射的时间顺序。目前获取此类药代动力学数据的方法包括:使用F - 18标记的硼化递送剂(例如对硼苯丙氨酸)进行正电子发射断层扫描、对血液(偶尔也对组织)样本进行体外中子活化分析以及核磁共振(NMR)技术。一般来说,由于B - 10和B - 11的大 quadrupole 矩以及(对于B - 10而言)非常低的旋磁比,再加上临床条件下这些同位素的生理浓度较低,NMR方法一直受到信噪比极低的阻碍。这项初步研究检验了质子NMR光谱用于此类应用的可行性。我们利用质子NMR光谱研究了在BNCT中遇到的典型生理浓度下对硼苯丙氨酸果糖(BPA - f)的可检测性。BPA - f是目前在美国、日本和欧洲正在进行临床I/II期试验的两种硼递送剂之一。这项研究包括对BPA - f进行高分辨率1H光谱表征,以识别用于检测和定量的有用光谱特征。该研究考察了潜在干扰,证明了NMR信号响应与浓度呈线性关系,并展示了体外血液样本和体内脑组织中的BPA NMR光谱。

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