Abstract

Fiber-reinforced load-bearing soft tissues, including tendon, meniscus, and annulus fibrosus, have hierarchical structure and biochemical composition that enables in vivo mechanical function. These tissues are prone to degeneration and injury, with debilitating consequences, high costs, and limited therapeutic options. Although load-bearing tissues are classically described using idealized schematics showing an ordered prevailing fiber direction, these tissues are in fact highly inhomogeneous, with amorphous proteoglycan-rich structural micro-domains within an otherwise ordered collagen-rich fibrous tissue - they are not simply a schematic. The objective of this proposal is to investigate micro-level structure-function of native and engineered tissue by quantifying and modeling mechanics from the tissue to the cellular level, and evaluating the mechanistic impact of micro-level structure-function on mechanotransduction. This study will also recapitulate these natural and/or potentially diseased micro-environments in engineered tissues in order to develop controlled in vitro systems to evaluate altered mechanotransduction. Quantifying the size, mechanical inhomogeneity, and biological response among tissue micro-domains is important because this is the length scale that governs cell mechanotransduction, and therefore regulation of tissue homeostasis and disease progression. These studies will advance the field of regenerative medicine by addressing micromechanical mechanisms in tissue development, degeneration, and injury. Ultimately, this new understanding will direct therapeutic strategies for rehabilitatio, repair, and replacement to promote and preserve healthy mechanotransduction in fibrous load bearing tissues.

Public Health Relevance

Load-bearing soft tissues, including tendon, meniscus, and annulus fibrosus, have a fiber-reinforced structure that enables mechanical function. These tissues are prone to degeneration and injury, with debilitating consequences, high costs, and limited therapeutic options. This proposal will investigate micro-level structure-function (?S/F) o native and engineered tissue by quantifying and modeling mechanics from the macroscopic to the cellular (micro-domain) level and evaluating the impact of ?S/F on cell mechanotransduction. These relationships are critical, as cell mechanotransduction and regulation of tissue homeostasis and disease progression occurs at this length scale. Ultimately, this new understanding will direct therapeutic strategies for rehabilitation, repair, and replacement to promote and preserve healthy mechanotransduction in fibrous load bearing tissues.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Biomedical Imaging and Bioengineering (NIBIB)
Type
Research Project (R01)
Project #
5R01EB002425-10
Application #
8822293
Study Section
Skeletal Biology Structure and Regeneration Study Section (SBSR)
Program Officer
Hunziker, Rosemarie
Project Start
2003-09-30
Project End
2018-03-31
Budget Start
2015-04-01
Budget End
2016-03-31
Support Year
10
Fiscal Year
2015
Total Cost
$441,366
Indirect Cost
$66,085

  Institution

Name
University of Delaware
Department
Biomedical Engineering
Type
Schools of Engineering
DUNS #
059007500
City
Newark
State
DE
Country
United States
Zip Code
19716

  Publications

Li, Qing; Wang, Chao; Han, Biao et al. (2018) Impacts of maturation on the micromechanics of the meniscus extracellular matrix. J Biomech 72:252-257
Szczesny, Spencer E; Aeppli, CĂ©line; David, Alexander et al. (2018) Fatigue loading of tendon results in collagen kinking and denaturation but does not change local tissue mechanics. J Biomech 71:251-256
Heo, Su-Jin; Szczesny, Spencer E; Kim, Dong Hwa et al. (2018) Expansion of mesenchymal stem cells on electrospun scaffolds maintains stemness, mechano-responsivity, and differentiation potential. J Orthop Res 36:808-815
Li, Qing; Qu, Feini; Han, Biao et al. (2017) Micromechanical anisotropy and heterogeneity of the meniscus extracellular matrix. Acta Biomater 54:356-366
Safa, Babak N; Meadows, Kyle D; Szczesny, Spencer E et al. (2017) Exposure to buffer solution alters tendon hydration and mechanics. J Biomech 61:18-25
Lee, Andrea H; Elliott, Dawn M (2017) Freezing does not alter multiscale tendon mechanics and damage mechanisms in tension. Ann N Y Acad Sci 1409:85-94
Szczesny, Spencer E; Mauck, Robert L (2017) The Nuclear Option: Evidence Implicating the Cell Nucleus in Mechanotransduction. J Biomech Eng 139:
Szczesny, Spencer E; Fetchko, Kristen L; Dodge, George R et al. (2017) Evidence that interfibrillar load transfer in tendon is supported by small diameter fibrils and not extrafibrillar tissue components. J Orthop Res 35:2127-2134
Peloquin, John M; Santare, Michael H; Elliott, Dawn M (2016) Advances in Quantification of Meniscus Tensile Mechanics Including Nonlinearity, Yield, and Failure. J Biomech Eng 138:021002
Heo, Su-Jin; Driscoll, Tristan P; Thorpe, Stephen D et al. (2016) Differentiation alters stem cell nuclear architecture, mechanics, and mechano-sensitivity. Elife 5:

Showing the most recent 10 out of 52 publications