Determination of spinal tracer dispersion after intrathecal injection in a deformable CNS model

Ayankola O Ayansiji; Daniel S Gehrke; Bastien Baralle; Ariel Nozain; Meenesh R Singh; Andreas A Linninger

doi:10.3389/fphys.2023.1244016

Determination of spinal tracer dispersion after intrathecal injection in a deformable CNS model

Front Physiol. 2023 Sep 25:14:1244016. doi: 10.3389/fphys.2023.1244016. eCollection 2023.

Authors

Ayankola O Ayansiji^{1

2}, Daniel S Gehrke¹, Bastien Baralle³, Ariel Nozain³, Meenesh R Singh², Andreas A Linninger^{1

4}

Affiliations

¹ Department of Bioengineering, University of Illinois Chicago, Chicago, IL, United States.
² Department of Chemical Engineering, University of Illinois Chicago, Chicago, IL, United States.
³ UIC Student Intern From EPF, Ecole D'Ingénieur, Paris, France.
⁴ Department of Neurosurgery, University of Illinois Chicago, Chicago, IL, United States.

Abstract

Background: Traditionally, there is a widely held belief that drug dispersion after intrathecal (IT) delivery is confined locally near the injection site. We posit that high-volume infusions can overcome this perceived limitation of IT administration. Methods: To test our hypothesis, subject-specific deformable phantom models of the human central nervous system were manufactured so that tracer infusion could be realistically replicated in vitro over the entire physiological range of pulsating cerebrospinal fluid (CSF) amplitudes and frequencies. The distribution of IT injected tracers was studied systematically with high-speed optical methods to determine its dependence on injection parameters (infusion volume, flow rate, and catheter configurations) and natural CSF oscillations in a deformable model of the central nervous system (CNS). Results: Optical imaging analysis of high-volume infusion experiments showed that tracers spread quickly throughout the spinal subarachnoid space, reaching the cervical region in less than 10 min. The experimentally observed biodispersion is much slower than suggested by the Taylor-Aris dispersion theory. Our experiments indicate that micro-mixing patterns induced by oscillatory CSF flow around microanatomical features such as nerve roots significantly accelerate solute transport. Strong micro-mixing effects due to anatomical features in the spinal subarachnoid space were found to be active in intrathecal drug administration but were not considered in prior dispersion theories. Their omission explains why prior models developed in the engineering community are poor predictors for IT delivery. Conclusion: Our experiments support the feasibility of targeting large sections of the neuroaxis or brain utilizing high-volume IT injection protocols. The experimental tracer dispersion profiles acquired with an anatomically accurate, deformable, and closed in vitro human CNS analog informed a new predictive model of tracer dispersion as a function of physiological CSF pulsations and adjustable infusion parameters. The ability to predict spatiotemporal dispersion patterns is an essential prerequisite for exploring new indications of IT drug delivery that targets specific regions in the CNS or the brain.

Keywords: drug infusion parameters; geometry-induced mixing; in vitro deformable spine model; intrathecal drug delivery; method of moments; oscillatory CSF flow.

Abstract

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