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利用脑脊液循环将药物递送到脑组织。

Harnessing cerebrospinal fluid circulation for drug delivery to brain tissues.

机构信息

AbbVie Inc., 1 N Waukegan Road, North Chicago, IL 60064, USA.

Departments of Neurosurgery and Bioengineering, University of Illinois at Chicago, Chicago, IL 60612, USA.

出版信息

Adv Drug Deliv Rev. 2021 Jun;173:20-59. doi: 10.1016/j.addr.2021.03.002. Epub 2021 Mar 9.

Abstract

Initially thought to be useful only to reach tissues in the immediate vicinity of the CSF circulatory system, CSF circulation is now increasingly viewed as a viable pathway to deliver certain therapeutics deeper into brain tissues. There is emerging evidence that this goal is achievable in the case of large therapeutic proteins, provided conditions are met that are described herein. We show how fluid dynamic modeling helps predict infusion rate and duration to overcome high CSF turnover. We posit that despite model limitations and controversies, fluid dynamic models, pharmacokinetic models, preclinical testing, and a qualitative understanding of the glymphatic system circulation can be used to estimate drug penetration in brain tissues. Lastly, in addition to highlighting landmark scientific and medical literature, we provide practical advice on formulation development, device selection, and pharmacokinetic modeling. Our review of clinical studies suggests a growing interest for intra-CSF delivery, particularly for targeted proteins.

摘要

最初认为脑脊液循环系统仅对临近的组织有用,但现在越来越多的人认为它是一种将某些治疗药物输送到脑组织深部的可行途径。有新的证据表明,对于大的治疗性蛋白质,如果满足本文所述的条件,这一目标是可以实现的。我们展示了如何通过流体动力学模型来帮助预测输注速度和时间,以克服高脑脊液周转率。我们假设,尽管存在模型限制和争议,但流体动力学模型、药代动力学模型、临床前测试以及对糖质淋系统循环的定性理解,可以用于估计药物在脑组织中的渗透情况。最后,除了强调标志性的科学和医学文献外,我们还就制剂开发、设备选择和药代动力学模型提供了实用建议。我们对临床研究的综述表明,人们对脑室内给药越来越感兴趣,特别是针对靶向蛋白的治疗。

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