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硼中子俘获治疗的放射生物学

The radiation biology of boron neutron capture therapy.

作者信息

Coderre J A, Morris G M

机构信息

Medical Department, Brookhaven National Laboratory, Upton, New York 11973, USA.

出版信息

Radiat Res. 1999 Jan;151(1):1-18.

PMID:9973079
Abstract

Boron neutron capture therapy (BNCT) is a targeted radiation therapy that significantly increases the therapeutic ratio relative to conventional radiotherapeutic modalities. BNCT is a binary approach: A boron-10 (10B)-labeled compound is administered that delivers high concentrations of 10B to the target tumor relative to surrounding normal tissues. This is followed by irradiation with thermal neutrons or epithermal neutrons which become thermalized at depth in tissues. The short range (5-9 microm) of the alpha and 7Li particles released from the 10B(n,alpha)7Li neutron capture reaction make the microdistribution of 10B of critical importance in therapy. The radiation field in tissues during BNCT consists of a mixture of components with differing LET characteristics. Studies have been carried out in both normal and neoplastic tissues to characterize the relative biological effectiveness of each radiation component. The distribution patterns and radiobiological characteristics of the two 10B delivery agents in current clinical use, the amino acid p-boronophenylalanine (BPA) and the sulfhydryl borane (BSH), have been evaluated in a range of normal tissues and tumor types. Considered overall, BSH-mediated BNCT elicits proportionately less damage to normal tissue than does BNCT mediated with BPA. However, BPA exhibits superior in vivo tumor targeting and has proven much more effective in the treatment of brain tumors in rats. In terms of fractionation effects, boron neutron capture irradiation modalities are comparable with other high-LET radiation modalities such as fast-neutron therapy. There was no appreciable advantage in increasing the number of daily fractions of thermal neutrons beyond two with regard to sparing of normal tissue in the rat spinal cord model. The experimental studies described in this review constitute the radiobiological basis for the new BNCT clinical trials for glioblastoma at Brookhaven National Laboratory, at the Massachusetts Institute of Technology, and at the High Flux Reactor, Petten, The Netherlands. The radiobiology of experimental and clinical BNCT is discussed in detail.

摘要

硼中子俘获疗法(BNCT)是一种靶向放射疗法,相对于传统放射治疗方式,它能显著提高治疗比率。BNCT采用二元方法:给予一种硼 - 10(¹⁰B)标记的化合物,该化合物相对于周围正常组织,能将高浓度的¹⁰B递送至靶肿瘤。随后用热中子或超热中子进行照射,这些中子在组织深部会热化。¹⁰B(n,α)⁷Li中子俘获反应释放的α粒子和⁷Li粒子射程较短(5 - 9微米),这使得¹⁰B的微观分布在治疗中至关重要。BNCT期间组织中的辐射场由具有不同传能线密度(LET)特征的成分混合而成。已在正常组织和肿瘤组织中开展研究,以表征每种辐射成分的相对生物效应。目前临床使用的两种¹⁰B递送剂,即氨基酸对硼苯丙氨酸(BPA)和巯基硼烷(BSH),在一系列正常组织和肿瘤类型中的分布模式及放射生物学特性已得到评估。总体而言,与BPA介导的BNCT相比,BSH介导的BNCT对正常组织造成的损伤相对较小。然而,BPA在体内肿瘤靶向方面表现更优,并且已证明在大鼠脑肿瘤治疗中效果更佳。就分次照射效应而言,硼中子俘获照射方式与其他高LET辐射方式(如快中子疗法)相当。在大鼠脊髓模型中,将热中子每日分次次数增加到两次以上,在保护正常组织方面并无明显优势。本综述中描述的实验研究构成了布鲁克海文国家实验室、麻省理工学院以及荷兰佩滕高通量反应堆针对胶质母细胞瘤开展的新型BNCT临床试验的放射生物学基础。本文将详细讨论实验性和临床BNCT的放射生物学。

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