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使用新型脑脊液系统模拟物对人体鞘内溶质转运动力学进行研究。

Investigation of Human Intrathecal Solute Transport Dynamics Using a Novel Cerebrospinal Fluid System Analog.

作者信息

Seiner Akari, Burla Goutham Kumar Reddy, Shrestha Dev, Bowen Mayumi, Horvath Joshua D, Martin Bryn A

机构信息

Department of Chemical and Biological Engineering, University of Idaho, Moscow, ID, United States.

Genentech, Inc., A Member of the Roche Group, South San Francisco, CA, United States.

出版信息

Front Neuroimaging. 2022 Jun 23;1:879098. doi: 10.3389/fnimg.2022.879098. eCollection 2022.

Abstract

BACKGROUND

Understanding the relationship between cerebrospinal fluid (CSF) dynamics and intrathecal drug delivery (ITDD) injection parameters is essential to improve treatment of central nervous system (CNS) disorders.

METHODS

An anatomically detailed model of the complete CSF system was constructed. Patient-specific cardiac- and respiratory-induced CSF oscillations were input to the model in the subarachnoid space and within the ventricles. CSF production was input at the lateral ventricles and CSF absorption at the superior sagittal sinus. A model small molecule simulated drug product containing fluorescein was imaged within the system over a period of 3-h post-lumbar ITDD injections and used to quantify the impact of (a) bolus injection volume and rate, (b) post-injection flush volume, rate, and timing, (c) injection location, and (d) type of injection device. For each experiment, neuraxial distribution of fluorescein in terms of spatial temporal concentration, area-under-the-curve (AUC), and percent of injected dose (%ID) to the brain was quantified at a time point 3-h post-injection.

RESULTS

For all experiments conducted with ITDD administration in the lumbar spine, %ID to the brain did not exceed 11.6% at a time point 3-h post-injection. Addition of a 12 mL flush slightly increased solute transport to the brain up to +3.9%ID compared to without a flush ( < 0.01). Implantation of a lumbar catheter with the tip at an equivalent location to the lumbar placed needle, but with rostral tip orientation, resulted in a small improvement of 1.5%ID to the brain ( < 0.05). An increase of bolus volume from 5 to 20 mL improved solute transport to the brain from 5.0 to 6.3%ID, but this improvement was not statistically significant. Increasing bolus injection rate from 5 to 13.3 mL/min lacked improvement of solute transport to the brain, with a value of 6.3 compared to 5.7%ID.

CONCLUSION

The modeling approach allowed precisely controlled and repeatable parametric investigation of ITDD injection protocols and devices. In combination, the results predict that parametric changes in lumbar spine ITDD-injection related parameters and devices can alter %ID to the brain and be tuned to optimize therapeutic benefit to CNS targets.

摘要

背景

了解脑脊液(CSF)动力学与鞘内药物递送(ITDD)注射参数之间的关系对于改善中枢神经系统(CNS)疾病的治疗至关重要。

方法

构建了一个完整CSF系统的详细解剖模型。将特定患者的心脏和呼吸引起的CSF振荡输入到蛛网膜下腔和脑室内的模型中。在侧脑室输入CSF生成量,在上矢状窦输入CSF吸收量。在腰椎ITDD注射后3小时内,对系统内含有荧光素的模型小分子模拟药物产品进行成像,并用于量化(a)推注注射体积和速率、(b)注射后冲洗体积、速率和时间、(c)注射位置以及(d)注射装置类型的影响。对于每个实验,在注射后3小时的时间点,根据空间时间浓度、曲线下面积(AUC)以及向脑内的注射剂量百分比(%ID)对荧光素的神经轴分布进行量化。

结果

对于所有在腰椎进行ITDD给药的实验,注射后3小时时间点向脑内的%ID不超过11.6%。与不冲洗相比,添加12 mL冲洗液可使溶质向脑内的转运略有增加,最高可达+3.9%ID(<0.01)。将腰椎导管尖端植入与腰椎穿刺针等效位置但尖端朝头侧的位置,可使向脑内的%ID略有提高1.5%(<0.05)。推注体积从5 mL增加到20 mL可使溶质向脑内的转运从5.0%ID提高到6.3%ID,但这种提高无统计学意义。推注注射速率从5 mL/min增加到13.3 mL/min并未改善溶质向脑内的转运,分别为6.3%ID和5.7%ID。

结论

该建模方法允许对ITDD注射方案和装置进行精确控制和可重复的参数研究。综合来看,结果预测腰椎ITDD注射相关参数和装置的参数变化可改变向脑内的%ID,并可进行调整以优化对CNS靶点的治疗效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1358/10406265/0fec2c26027a/fnimg-01-879098-g0001.jpg

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