Overcoming the blood-brain barrier in primary central nervous system lymphoma: a review on new strategies to solve an old problem

T. Calimeri, F. Marcucci, A. Corti
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引用次数: 4

Abstract

A great deal of research is being dedicated to the identification of new strategies to improve the transport of medicines across the blood-brain barrier (BBB), which typically hampers the transport of molecules and particles into the brain. Primary DLBCL of the CNS (PCNSL) is a paradigmatic example of this challenge both from a diagnostic and therapeutic point of view. PCNSL is a neoplasm confined to the brain, eyes, meninges, and other structures of the CNS. Histopathologic analyses of tissue sections have demonstrated that tumor cells can be detected not only in the areas highlighted by modern neuroimaging, but also far from these zones. Furthermore, some tumor areas revealed by gadolinium-enhanced MRI are concomitant with histological lesions with only T2-weighted-fluid-attenuated inversion recovery (FLAIR) changes, or with no radiologic abnormalities at all, suggesting the presence of a blood-brain tumor barrier (BBTB) heterogeneously altered in PCNSL, or even intact in some tumor areas. Since the unaltered barrier may impair the homogeneous penetration of low-molecular weight MRI contrast agents and therapeutic compounds in tumors, this issue represents an important diagnostic and therapeutic challenge. Based on these considerations, the induction of BBTB permeabilization to enhance tumor penetration of drugs and molecules could be attractive investigational approaches in this setting. The aim of this review article is to report and critically discuss the strategies recently developed to overcome this obstacle in PCNSL patients, with a special focus on the use of targeted tumor necrosis factor-alpha (TNF) to enhance CNS bioavailability of therapeutic agents.
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克服原发性中枢神经系统淋巴瘤的血脑屏障:解决老问题的新策略综述
大量的研究正在致力于确定新的策略来改善药物通过血脑屏障(BBB)的运输,这通常会阻碍分子和颗粒进入大脑的运输。从诊断和治疗的角度来看,原发性中枢神经系统DLBCL (PCNSL)是这一挑战的典型例子。PCNSL是一种局限于大脑、眼睛、脑膜和中枢神经系统其他结构的肿瘤。组织切片的组织病理学分析表明,肿瘤细胞不仅可以在现代神经成像突出的区域检测到,而且可以在远离这些区域的区域检测到。此外,一些钆增强MRI显示的肿瘤区域伴有组织学病变,只有t2加权液体衰减反转恢复(FLAIR)改变,或根本没有放射学异常,提示PCNSL存在血脑肿瘤屏障(BBTB)异质性改变,甚至在某些肿瘤区域完整。由于未改变的屏障可能会破坏低分子量MRI造影剂和治疗化合物在肿瘤中的均匀渗透,这一问题代表了一个重要的诊断和治疗挑战。基于这些考虑,诱导BBTB透性以增强药物和分子对肿瘤的渗透可能是在这种情况下有吸引力的研究方法。这篇综述文章的目的是报道和批判性地讨论最近开发的策略,以克服PCNSL患者的这一障碍,特别关注使用靶向肿瘤坏死因子- α (TNF)来提高治疗药物的中枢神经系统生物利用度。
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