A Spatial Interpolation Approach to Assign Magnetic Resonance Imaging-Derived Material Properties for Finite Element Models of Adeno-Associated Virus Infusion Into a Recurrent Brain Tumor

Author:

Chen Reed1ORCID,Rey Julian A.23,Tuna Ibrahim S.43,Tran David D.56,Sarntinoranont Malisa7

Affiliation:

1. Department of Biomedical Engineering, Duke University , 407 Towerview Rd, Box 97756 , Durham, NC 27708

2. Department of Mechanical & Aerospace Engineering, University of Florida , 142 New Engineering Building, P.O. Box 116250 , Gainesville, FL 32611

3. University of Florida

4. Department of Radiology, University of Florida College of Medicine , P.O. Box 100374 , Gainesville, FL 32610-0374

5. Division of Neuro-Oncology, Department of Neurological Surgery and Neurology USC Brain Tumor Center, University of Southern California Keck School of Medicine , Los Angeles, CA 90033

6. University of Southern California

7. Department of Mechanical & Aerospace Engineering, University of Florida , 497 Wertheim, P.O. Box 116250 , Gainesville, FL 32611

Abstract

Abstract Adeno-associated virus (AAV) is a clinically useful gene delivery vehicle for treating neurological diseases. To deliver AAV to focal targets, direct infusion into brain tissue by convection-enhanced delivery (CED) is often needed due to AAV's limited penetration across the blood-brain-barrier and its low diffusivity in tissue. In this study, computational models that predict the spatial distribution of AAV in brain tissue during CED were developed to guide future placement of infusion catheters in recurrent brain tumors following primary tumor resection. The brain was modeled as a porous medium, and material property fields that account for magnetic resonance imaging (MRI)-derived anatomical regions were interpolated and directly assigned to an unstructured finite element mesh. By eliminating the need to mesh complex surfaces between fluid regions and tissue, mesh preparation was expedited, increasing the model's clinical feasibility. The infusion model predicted preferential fluid diversion into open fluid regions such as the ventricles and subarachnoid space (SAS). Additionally, a sensitivity analysis of AAV delivery demonstrated that improved AAV distribution in the tumor was achieved at higher tumor hydraulic conductivity or lower tumor porosity. Depending on the tumor infusion site, the AAV distribution covered 3.67–70.25% of the tumor volume (using a 10% AAV concentration threshold), demonstrating the model's potential to inform the selection of infusion sites for maximal tumor coverage.

Publisher

ASME International

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