To quantify the transport and adhesion of drug particles in a complex vascular environment, computational fluid particle dynamics (CFPD) simulations of blood flow and drug particulate were conducted in three different geometries representing the human lung vasculature for steady and pulsatile flow conditions. A fully developed flow profile was assumed as the inlet velocity, and a lumped mathematical model was used for the calculation of the outlet pressure boundary condition. A receptor–ligand model was used to simulate the particle binding probability. The results indicate that bigger particles have lower deposition fraction due to less chance of successful binding. Realistic unsteady flow significantly accelerates the binding activity over a wide range of particle sizes and also improves the particle deposition fraction in bifurcation regions when comparing with steady flow condition. Furthermore, surface imperfections and geometrical complexity coupled with the pulsatility effect can enhance fluid mixing and accordingly particle binding efficiency. The particle binding density at bifurcation regions increases with generation order and drug carriers are washed away faster in steady flow. Thus, when studying drug delivery mechanism in vitro and in vivo, it is important to take into account blood flow pulsatility in realistic geometry. Moreover, tissues close to bifurcations are more susceptible to deterioration due to higher uptake.
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December 2014
Research-Article
Numerical Simulation of Particle Transport and Deposition in the Pulmonary Vasculature
Salman Sohrabi,
Salman Sohrabi
Department of Mechanical
Engineering & Mechanics,
e-mail: Sas713@Lehigh.edu
Engineering & Mechanics,
Lehigh University
,Bethlehem, PA 18015
e-mail: Sas713@Lehigh.edu
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Junda Zheng,
Junda Zheng
Department of Mechanical
Engineering and Mechanics,
e-mail: Juz212@Lehigh.edu
Engineering and Mechanics,
Lehigh University
,Bethlehem, PA 18015
e-mail: Juz212@Lehigh.edu
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Ender A. Finol,
Ender A. Finol
Department of Biomedical Engineering,
The University of Texas at
e-mail: Ender.finol@utsa.edu
The University of Texas at
San Antonio
, TX 78249
e-mail: Ender.finol@utsa.edu
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Yaling Liu
Yaling Liu
1
Mem. ASME
Department of Mechanical
Engineering & Mechanics,
e-mail: Yal310@lehigh.edu
Department of Mechanical
Engineering & Mechanics,
Bioengineering Program Lehigh University
,Bethlehem, PA 18015
e-mail: Yal310@lehigh.edu
1Corresponding author.
Search for other works by this author on:
Salman Sohrabi
Department of Mechanical
Engineering & Mechanics,
e-mail: Sas713@Lehigh.edu
Engineering & Mechanics,
Lehigh University
,Bethlehem, PA 18015
e-mail: Sas713@Lehigh.edu
Junda Zheng
Department of Mechanical
Engineering and Mechanics,
e-mail: Juz212@Lehigh.edu
Engineering and Mechanics,
Lehigh University
,Bethlehem, PA 18015
e-mail: Juz212@Lehigh.edu
Ender A. Finol
Department of Biomedical Engineering,
The University of Texas at
e-mail: Ender.finol@utsa.edu
The University of Texas at
San Antonio
, TX 78249
e-mail: Ender.finol@utsa.edu
Yaling Liu
Mem. ASME
Department of Mechanical
Engineering & Mechanics,
e-mail: Yal310@lehigh.edu
Department of Mechanical
Engineering & Mechanics,
Bioengineering Program Lehigh University
,Bethlehem, PA 18015
e-mail: Yal310@lehigh.edu
1Corresponding author.
Manuscript received April 21, 2014; final manuscript received October 6, 2014; accepted manuscript posted October 15, 2014; published online November 7, 2014. Assoc. Editor: Naomi Chesler.
J Biomech Eng. Dec 2014, 136(12): 121010 (11 pages)
Published Online: December 1, 2014
Article history
Received:
April 21, 2014
Revision Received:
October 6, 2014
Accepted:
October 15, 2014
Citation
Sohrabi, S., Zheng, J., Finol, E. A., and Liu, Y. (December 1, 2014). "Numerical Simulation of Particle Transport and Deposition in the Pulmonary Vasculature." ASME. J Biomech Eng. December 2014; 136(12): 121010. https://doi.org/10.1115/1.4028800
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