Abstract

Vascular growth and remodeling (G&R) plays a key role in many physiological (e.g., normal vascular development and aging) and pathophysiological processes (e.g., hypertension, arteriosclerosis, and aneurysms), as well as the success (or failure) of many clinical interventions (e.g., vein grafts, synthetic vascular grafts, stents, and balloon angioplasty). Despite the explosion of information on soft tissue G&R, from molecular level to the tissue and whole organism level, attempts at integrating these data into a predictive model is still in its infancy. The goal of the current proposal is to develop and test an innovative theoretical- experimental paradigm for characterizing the time-course of vascular remodeling that integrates a novel organ culture device, two-photon laser scanning microscopy (LSM), biaxial biomechanical testing, and multi-scale mathematical modeling. Our central hypothesis is that volume fractions, fiber directions, and stress-free states of elastic fibers, collagen fibers, and smooth muscle cells can be quantified via two-photon LSM in parallel with biaxial biomechanical data on live mouse CCAs and these data can be incorporated into a constrained mixture model to describe and predict temporal changes in material behavior in both normal (adaptive) and maladaptive remodeling. Whereas much attention has been paid to the role of wall shear stress and circumferential (hoop) stress in vascular remodeling, the role of axial stress has been largely overlooked. Many clinical observations, however, highlight the importance of axial remodeling in the vasculature; marked tortuousity in AAAs, mammary artery by-pass grafts, and many vessels with hypertension and aging are a few but a few examples. Elastic fibers are thought to endow arteries with their in vivo axial stain and the loss of functional elastic fibers (which occurs aneurysms, hypertension, and aging) may be associated with impaired axial remodeling and development of tortuousity. Fibulin-5 is an ECM protein that binds tropoelastin and fibrillins with ava3, ava5, and a9a1 integrins(60) to bridge elastic fibers with cells. Thus, fibulin-5 is likely a key protein involved in regulation of elastic fibers and thus key in axial remodeling.
The aims of this proposal are to measure and characterize the biomechanical behavior and microstructural organization of CCAs from wild-type and fib-5-/- mice and observe and quantify the biomechanical and microstructural remodeling of CCAs from wild-type and fib-5-/- mice exposed to (a) increased axial extension (b) increase transmural pressure, or (c) combined increase in axial extension and pressure in organ culture. Successful realization of these aims will establish an innovative approach for studying vascular remodeling under normal and pathophysiological conditions that can be used gain insights toward the development clinical pathologies and the design of appropriate clinical interventions. Vascular remodeling plays a key role in many physiological (e.g., normal vascular development and aging) and pathophysiological processes (e.g., hypertension, arteriosclerosis, and aneurysms), as well as the success (or failure) of many clinical interventions (e.g., vein grafts, synthetic vascular grafts, stents, and balloon angioplasty). The purpose of this work is to develop an innovative approach for studying vascular remodeling that combines multi-scale computational modeling with tissue culture and multi-photon microscopy that can be used gain insights toward the development clinical pathologies and the design of appropriate clinical interventions. ? ? ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Exploratory/Developmental Grants (R21)
Project #
5R21HL085822-02
Application #
7499745
Study Section
Hypertension and Microcirculation Study Section (HM)
Program Officer
Reid, Diane M
Project Start
2007-09-24
Project End
2010-06-30
Budget Start
2008-07-01
Budget End
2010-06-30
Support Year
2
Fiscal Year
2008
Total Cost
$181,791
Indirect Cost

  Institution

Name
Georgia Institute of Technology
Department
Engineering (All Types)
Type
Schools of Engineering
DUNS #
097394084
City
Atlanta
State
GA
Country
United States
Zip Code
30332

  Publications

Hansen, Laura; Parker, Ivana; Roberts, LaDeidra Monet et al. (2013) Azidothymidine (AZT) leads to arterial stiffening and intima-media thickening in mice. J Biomech 46:1540-7
Wang, Ruoya; Brewster, Luke P; Gleason Jr, Rudolph L (2013) In-situ characterization of the uncrimping process of arterial collagen fibers using two-photon confocal microscopy and digital image correlation. J Biomech 46:2726-9
Hansen, Laura; Parker, Ivana; Sutliff, Roy L et al. (2013) Endothelial dysfunction, arterial stiffening, and intima-media thickening in large arteries from HIV-1 transgenic mice. Ann Biomed Eng 41:682-93
Wan, William; Yanagisawa, Hiromi; Gleason Jr, Rudolph L (2010) Biomechanical and microstructural properties of common carotid arteries from fibulin-5 null mice. Ann Biomed Eng 38:3605-17
Wan, William; Hansen, Laura; Gleason Jr, Rudolph L (2010) A 3-D constrained mixture model for mechanically mediated vascular growth and remodeling. Biomech Model Mechanobiol 9:403-19
Wang, Ruoya; Gleason Jr, Rudolph L (2010) A mechanical analysis of conduit arteries accounting for longitudinal residual strains. Ann Biomed Eng 38:1377-87
Rachev, Alexander (2009) A theoretical study of mechanical stability of arteries. J Biomech Eng 131:051006
Hansen, Laura; Wan, William; Gleason, Rudolph L (2009) Microstructurally motivated constitutive modeling of mouse arteries cultured under altered axial stretch. J Biomech Eng 131:101015