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评估注射方案对非人类灵长类动物鞘内溶质弥散的影响:使用食蟹猴脑脊液系统的体外研究。

Evaluating the effect of injection protocols on intrathecal solute dispersion in non-human primates: an in vitro study using a cynomolgus cerebrospinal fluid system.

机构信息

Department of Chemical and Biological Engineering, University of Idaho, 875 Perimeter Dr. MC1122, Moscow, ID, 83844, USA.

Genentech, Inc., a member of the Roche Group, South San Francisco, CA, USA.

出版信息

Fluids Barriers CNS. 2024 Jul 26;21(1):61. doi: 10.1186/s12987-024-00556-2.

Abstract

BACKGROUND

Achieving effective drug delivery to the central nervous system (CNS) remains a challenge for treating neurological disorders. Intrathecal (IT) delivery, which involves direct injection into the cerebrospinal fluid (CSF), presents a promising strategy. Large animal studies are important to assess the safety and efficacy of most drugs and treatments and translate the data to humans. An understanding of the influence of IT injection parameters on solute distribution within the CNS is essential to optimize preclinical research, which would potentially help design human clinical studies.

METHODS

A three-dimensional (3D) in vitro model of a cynomolgus monkey, based on MRI data, was developed to evaluate the impact of lumbar injection parameters on intrathecal solute dispersion. The parameters evaluated were (a) injection location, (b) bolus volume, (c) flush volume, (d) bolus rate, and (e) flush rate. To simulate the CSF flow within the subarachnoid space (SAS), an idealized CSF flow waveform with both cardiac and respiratory-induced components was input into the model. A solution of fluorescein drug surrogate tracer was administered in the lumbar region of the 3D in vitro model filled with deionized water. After injection of the tracer, the CSF system wide-solute dispersion was imaged using high-resolution cameras every thirty seconds for a duration of three hours. To ensure repeatability each injection protocol was repeated three times. For each protocol, the average spatial-temporal distribution over three hours post-injection, the area under the curve (AUC), and the percent injected dose (%ID) to extra-axial CSF (eaCSF) at three hours were determined.

RESULTS

The changes to the lumbar injection parameters led to variations in solute distribution along the neuro-axis. Specifically, injection location showed the most impact, enhancing the delivery to the eaCSF up to + 10.5%ID (p = 0.0282) at three hours post-injection. Adding a post-injection flush of 1.5 ml at 1 ml/min increased the solute delivery to the eaCSF by + 6.5%ID (p = 0.0218), while the larger bolus volume resulted in a + 2.3%ID (p = 0.1910) increase. The bolus and flush rates analyzed had minimal, statistically non-significant effects.

CONCLUSION

These results predict the effects of lumbar injection parameters on solute distribution in the intrathecal space in NHPs. Specifically, the choice of injection location, flush, and bolus volume significantly improved solute delivery to eaCSF. The in vitro NHP CSF model and results offer a system to help predict and optimize IT delivery protocols for pre-clinical NHP studies.

摘要

背景

将药物有效递送至中枢神经系统(CNS)仍然是治疗神经疾病的一项挑战。鞘内(IT)给药涉及直接将药物注入脑脊液(CSF)中,是一种很有前途的策略。大型动物研究对于评估大多数药物和治疗方法的安全性和有效性以及将数据转化为人类数据非常重要。了解 IT 注射参数对 CNS 内溶质分布的影响对于优化临床前研究至关重要,这可能有助于设计人体临床试验。

方法

根据 MRI 数据,开发了一种基于狨猴的 3D 体外模型,用于评估腰穿注射参数对鞘内溶质分散的影响。评估的参数包括:(a)注射位置;(b)推注体积;(c)冲洗体积;(d)推注速率;(e)冲洗速率。为了模拟蛛网膜下腔(SAS)内的 CSF 流动,将具有心脏和呼吸诱发成分的理想化 CSF 流动波形输入到模型中。在充满去离子水的 3D 体外模型的腰部区域注入荧光素药物示踪剂溶液。在注射示踪剂后,每隔 30 秒使用高分辨率相机对 CSF 系统进行全范围溶质扩散成像,持续 3 小时。为了确保重复性,每个注射方案重复三次。对于每个方案,确定注射后 3 小时内的平均时空分布、曲线下面积(AUC)和 3 小时时的外轴 CSF(eaCSF)中注入剂量的百分比(%ID)。

结果

腰椎注射参数的变化导致神经轴上溶质分布的变化。具体来说,注射位置的影响最大,可将药物递送至 eaCSF 的效率提高 10.5%ID(p=0.0282)。在注射后进行 1.5ml 冲洗液冲洗,可将溶质递送至 eaCSF 的效率提高 6.5%ID(p=0.0218),而更大的推注体积仅使效率提高 2.3%ID(p=0.1910)。分析的推注和冲洗速度影响最小,无统计学意义。

结论

这些结果预测了腰椎注射参数对 NHPs 鞘内空间中溶质分布的影响。具体来说,注射位置、冲洗液和推注体积的选择显著提高了 eaCSF 中的药物输送效率。该 NHPs 脑脊液体外模型及其结果提供了一个系统,有助于预测和优化临床前 NHPs 研究中的 IT 给药方案。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ffc/11282645/6008d48715df/12987_2024_556_Fig1_HTML.jpg

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