Publication: Optimized FDA Blood Pump: A Case Study in System-Level Customized Ventricular Assist Device Designs
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KU-Authors
KU Authors
Co-Authors
Yildirim, Canberk
Ucak, Ka an
Madayen, Ali
Golcez, Tansu
Erturk, Hakan
Baran, Ozgur Ugras
Pekkan, Kerem
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Abstract
Purpose The design and development of ventricular assist devices have heavily relied on computational tools, particularly computational fluid dynamics (CFD), since the early 2000s. However, traditional CFD-based optimization requires costly trial-and-error approaches involving multiple design cycles. This study aims to propose a more efficient VAD design and optimization framework that overcomes these limitations. Methods We developed a system- and component-level ventricle assist device optimization approach by coupling a lumped parameter cardiovascular physiology model with parametric turbomachinery, volute design, and blade path generation packages. The framework incorporates pump hydrodynamic losses and is validated against experimental data from six distinct blood pump designs and CFD simulations. The optimization framework allows for the specification of both physiology-related and device-related objective functions to generate optimized blood pump configurations over a large parameter space. Results The optimization was applied to the U.S. Food and Drug Administration (FDA) benchmark blood pump as the baseline design. Results showed that an optimized FDA pump, maintaining the same cardiac output and aortic pressure, achieved a similar to 32% reduction in blade tip velocity compared to the baseline, resulting in an similar to 88% reduction in hemolysis. Additionally, an alternative design with a 40% reduction in blood-wetted area was generated while preserving the baseline pressure and flow. Conclusion The proposed optimization framework improves device development efficiency by shortening the design cycle and enabling hydrodynamically optimized pumps that perform well across diverse patient hemodynamics. The optimized pump designs are available as open-source resources for further research and development.
Source
Publisher
SPRINGER
Subject
Engineering
Citation
Has Part
Source
ANNALS OF BIOMEDICAL ENGINEERING
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DOI
10.1007/s10439-025-03834-8
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Except where otherwised noted, this item's license is described as CC BY-NC-ND (Attribution-NonCommercial-NoDerivs)

