Contractile Three-Dimensional Bioengineered Heart Muscle for Myocardial Regeneration
Wiley Periodicas, Journal of Biomedical Materials Research (2006): 719-731
Yen-Chih Huang, Luda Khait, Ravi K. Birla
Department of Biomedical Engineering (Section of Cardiac Surgery), The University of Michigan, Ann Arbor, Michigan
Bioengineered heart muscle (BEHM) is being investigated as a method of treatment for early stage congestive heart failure. Various methods are currently under investigation including biodegradable gels/hydrogels and synthetic scaffolds. One of the biggest limitations of these methods is trying to provide a controllable mechanical environment for the engineered tissue that is a close match to the physiological environment of the native tissue; often the tissue constructs lack the necessary mechanical strength under physiological conditions.
This study investigated the use of a biodegradable fibrin gel as a novel method to engineer functional three-dimensional heart muscle. The fibrin gel functions as a support matrix to promote the formation of three-dimensional heart muscle, which forms from the self-organization of primary cardiac cells. The fibrin has the advantage that it has controllable degradation kinetics, so the rate of its degradation can be matched to the rate of tissue formation. This is important because it allows for the cardiac cells to organize into tissue and then allows for the gradual transfer of mechanical forces in the native environment from the matrix to the tissue.
Primary cardiac myocytes were isolated from newborn rats, and then two methods were used to form the BEHM: the layering method and the embedding method. With the layering approach, cells were plated on the surface of a tissue culture plate coated with PDMS, followed by thrombin and fibrin. In the second method, cells were suspended with thrombin and fibrin and then plated on PDMS tissue culture plates. Both approaches resulted in a three-dimensional tissue construct of cardiac tissue within seven days, and in both cases the monolayer of cardiac cells delaminated due to the spontaneous contraction of the cells.
Overall, the investigators found that the layering approach was better for myotube formation, which is necessary for the formation of cardiac tissue. The cardiac cells spread more, and the cell monolayer underwent spontaneous contractions with a consistent frequency that resembled the regular contractions of native myocardial tissue. The cells that were embedded in the fibrin gel didn’t spread as much, which is likely why only isolated patches of cells underwent contractions.
The investigators also looked at mechanical strength of the BEHMs generated via the two methods. The plating density didn’t affect the stimulated active force for the constructs produced via the embedded method, but the plating density did significantly affect the force for constructs that were produced via the layering method (the lower the density, the higher the forces). Additionally, the investigators found that by changing the media daily, they were able to maintain the stimulated active force for a period of two months. Unfortunately, these measured forces for the BEHMs was much lower compared to the specific force of native thin cardiac muscle.
Because my interests lie in tissue engineering, I found this paper interesting. In particular, it was exciting to me because it presents a rather new approach to generate engineered tissue; there has already been tremendous research investigating the use of synthetic scaffolds and hydrogels. Because this method is so novel there is a huge amount of research to be done, targeting some of the major problems (including the lower forces generated by BEHMs as compared to native cardiac tissue as mentioned earlier). Despite the limitations, this method is an exciting potential alternative to scaffolds and hydrogels in tissue engineering of cardiac muscle.
Wednesday, March 14, 2007
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5 comments:
The investigators also looked at mechanical strength of the BEHMs generated via the two methods."
I'm not quite clear on this. Are the two methods plating density and changing media? Or did they check mechanical strength in relation to these two things?
The investigators looked at the how the two methods of plating the cells with the fibrin to form the fibrin-gel affected the mechanical strength of the BEHM. In one method, the fibrin was added on top of plated cells, and in the other method the fibrin was suspended with cells and then plated.
In regards to Terry's question... I googled fibrin to read more about it and to try to find more specific answers to his questions. Fibrin is a protein that comes from fibrinogen during the formation of a blood clot. I wasn't able to find specifics about the rate of degradation of fibrin in vivo or the mechanism of degradation. Fibrin yields fibrin degradation products (what an original name), the effects of which are still being investigated.
One thing that I came across and found rather... interesting when I read more about fibrin is that higher levels of this protein is associated with heart disease... which makes this paper ironic conisdering the use the fibrin is being investigated for...
"Overall, the investigators found that the layering approach was better for myotube formation, which is necessary for the formation of cardiac tissue."
What exactly is the myotube formation and why is it necessary for the formation of cardiac tissue?
Wouldn't it be better if BEHMs were localized on a certain part suffering from ischemia than to spread out?
Wow, this paper is really fascinating...
"Unfortunately, these measured forces for the BEHMs was much lower compared to the specific force of native thin cardiac muscle."
How did they measure the force? Were all the myocytes beating in unison? I'm assuming for their suspended mycoyte model, if there were random contractions, then it was not, but what about the layering model?
A myotube is a developing muscle fiber with a tubular appearance. It's vital for the ultimate development of muscle.
The authors didn't really specify as to whether or not the BEHM would be localized to the ischemia. I think at this point most people are still investigating how they can create engineered heart muscle with the correct properties in the first place. Also, I think that following an infarction for instance, the heart overall is weakened. Using BEHM to help strengthen the heart would be beneficial.
To measure the contractile force, the authors used a micromanipulator (don't ask me- I'm not a mechanical engineer...) and a transducer to stimulate active force on the BEHM, and then measured the resulting cross-sectional area, which they normalized. I would suggest reading in the materials and methods to get a better explanation.
I don't know how the contractions affected the measurement of the force- the contractions of the muscle are what caused the BEHMs to delaminate, or lift, from the surface. The forces of these were then measured and compared to native heart tissue. Also, the authors didn't mention whether or not the cells were contracting in unison, or whether it was random, spontaneous contractions. I would assume, however, that because these contractions were what caused the BEHM to delaminate that the cells were contracting in unison in order to generate the necessary force.
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