scholarly journals Analysis and Demonstration of a Scaffold Finite Element Model for Cartilage Tissue Engineering

ACS Omega ◽  
2020 ◽  
Vol 5 (50) ◽  
pp. 32411-32419
Author(s):  
Kai Sun ◽  
Ruixin Li ◽  
Hui Li ◽  
Meng Fan ◽  
Hao Li
Keyword(s):  
Tissue Engineering ◽  
Finite Element ◽  
Finite Element Model ◽  
Cartilage Tissue Engineering ◽  
Element Model ◽  
Cartilage Tissue

Modeling Material-Degradation-Induced Elastic Property of Tissue Engineering Scaffolds

2010 ◽  
Vol 132 (11) ◽  
Author(s):  
N. K. Bawolin ◽  
M. G. Li ◽  
X. B. Chen ◽  
W. J. Zhang
Keyword(s):  
Mechanical Properties ◽  
Tissue Engineering ◽  
Molecular Weight ◽  
Finite Element ◽  
Finite Element Model ◽  
Model Updating ◽  
Element Model ◽  
Time Dependent ◽  
Tissue Engineering Scaffolds ◽  
The Finite Element Model

The mechanical properties of tissue engineering scaffolds play a critical role in the success of repairing damaged tissues/organs. Determining the mechanical properties has proven to be a challenging task as these properties are not constant but depend upon time as the scaffold degrades. In this study, the modeling of the time-dependent mechanical properties of a scaffold is performed based on the concept of finite element model updating. This modeling approach contains three steps: (1) development of a finite element model for the effective mechanical properties of the scaffold, (2) parametrizing the finite element model by selecting parameters associated with the scaffold microstructure and/or material properties, which vary with scaffold degradation, and (3) identifying selected parameters as functions of time based on measurements from the tests on the scaffold mechanical properties as they degrade. To validate the developed model, scaffolds were made from the biocompatible polymer polycaprolactone (PCL) mixed with hydroxylapatite (HA) nanoparticles and their mechanical properties were examined in terms of the Young modulus. Based on the bulk degradation exhibited by the PCL/HA scaffold, the molecular weight was selected for model updating. With the identified molecular weight, the finite element model developed was effective for predicting the time-dependent mechanical properties of PCL/HA scaffolds during degradation.

scholarly journals Dedifferentiation alters chondrocyte nuclear mechanics during in vitro culture and expansion

2021 ◽  
Author(s):  
Soham Ghosh ◽  
Adrienne K. Scott ◽  
Benjamin Seelbinder ◽  
Jeanne E. Barthold ◽  
Brittany M St. Martin ◽  
...  
Keyword(s):  
Gene Expression ◽  
Tissue Engineering ◽  
Finite Element ◽  
Nuclear Envelope ◽  
Cell Shape ◽  
Cartilage Tissue Engineering ◽  
Cartilage Tissue ◽  
Chondrocyte Phenotype ◽  
Nuclear Mechanics

ABSTRACTDedifferentiation of chondrocytes during in vitro passaging before implantation, and post implantation in vivo, is a critical limitation in cartilage tissue engineering. Several biophysical features define the dedifferentiated state including a flattened cell morphology and increased stress fiber formation. However, how dedifferentiation influences nuclear mechanics, and the possible long-term implications of this state, are unknown. In this study, we investigated how chondrocyte dedifferentiation affects the mechanics of the chromatin architecture inside the cell nucleus and the gene expression of the structural proteins located at the nuclear envelope. Through an experimental model of cell stretching and a detailed spatial intranuclear strain quantification, we identified that strain is amplified and distribution of strain within the chromatin is altered under tensile loading in the dedifferentiated state. Further, using a confocal microscopy image-based finite element model and simulation of cell stretching, we found that the cell shape is the primary determinant of the strain amplification inside the chondrocyte nucleus in the dedifferentiated state. Additionally, we found that nuclear envelope proteins have lower gene expression in the dedifferentiated state suggesting a weaker nuclear envelope which can further intensify the intranuclear strain amplification. Our results indicate that dedifferentiation and altered nuclear strain could promote gene expression changes at the nuclear envelope, thus promoting further deviation from chondrocyte phenotype. This study highlights the role of cell shape on nuclear mechanics and lays the groundwork to design biophysical strategies for the maintenance and enhancement of the chondrocyte phenotype during expansion with a goal of successful cartilage tissue engineering.SIGNIFICANCEChondrocytes dedifferentiate into a fibroblast-like phenotype in a non-native biophysical environment. Using high resolution microscopy, intranuclear strain analysis, finite element method based computational modeling, and molecular biology techniques, we investigated how mechanical force causes abnormal intranuclear strain distribution in chondrocytes during the dedifferentiation process. Overall, our results suggest that the altered cell geometry aided by an altered or weakened nuclear envelope structure are responsible for abnormal intranuclear strain during chondrocyte dedifferentiation that can further deviate chondrocytes to a more dedifferentiated state.

scholarly journals Utilization of Finite Element Analysis for Articular Cartilage Tissue Engineering

Materials ◽  
2019 ◽  
Vol 12 (20) ◽  
pp. 3331 ◽  
Author(s):  
Chaudhry R. Hassan ◽  
Yi-Xian Qin ◽  
David E. Komatsu ◽  
Sardar M.Z. Uddin
Keyword(s):  
Tissue Engineering ◽  
Finite Element Analysis ◽  
Finite Element ◽  
Articular Cartilage ◽  
Material Properties ◽  
Cartilage Tissue Engineering ◽  
Cartilage Tissue ◽  
Scaffold Design ◽  
Element Analysis ◽  
In Vivo Models

Scaffold design plays an essential role in tissue engineering of articular cartilage by providing the appropriate mechanical and biological environment for chondrocytes to proliferate and function. Optimization of scaffold design to generate tissue-engineered cartilage has traditionally been conducted using in-vitro and in-vivo models. Recent advances in computational analysis allow us to significantly decrease the time and cost of scaffold optimization using finite element analysis (FEA). FEA is an in-silico analysis technique that allows for scaffold design optimization by predicting mechanical responses of cells and scaffolds under applied loads. Finite element analyses can potentially mimic the morphology of cartilage using mesh elements (tetrahedral, hexahedral), material properties (elastic, hyperelastic, poroelastic, composite), physiological loads by applying loading conditions (static, dynamic), and constitutive stress–strain equations (linear, porous–elastic, biphasic). Furthermore, FEA can be applied to the study of the effects of dynamic loading, material properties cell differentiation, cell activity, scaffold structure optimization, and interstitial fluid flow, in isolated or combined multi-scale models. This review covers recent studies and trends in the use of FEA for cartilage tissue engineering and scaffold design.

Finite Element Simulation of Tire-Rim Interface

1989 ◽  
Vol 17 (4) ◽  
pp. 305-325 ◽  
Author(s):  
N. T. Tseng ◽  
R. G. Pelle ◽  
J. P. Chang
Keyword(s):  
Finite Element ◽  
Finite Element Model ◽  
Finite Element Simulation ◽  
Contact Pressure ◽  
Element Model ◽  
Experimental Measurements ◽  
Inflation Pressure ◽  
Interference Fit ◽  
Element Simulation ◽  
Rubber Composite

Abstract A finite element model was developed to simulate the tire-rim interface. Elastomers were modeled by nonlinear incompressible elements, whereas plies were simulated by cord-rubber composite elements. Gap elements were used to simulate the opening between tire and rim at zero inflation pressure. This opening closed when the inflation pressure was increased gradually. The predicted distribution of contact pressure at the tire-rim interface agreed very well with the available experimental measurements. Several variations of the tire-rim interference fit were analyzed.

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